pioglitazone and Body Weight studies

Pioglitazone: A thiazolidinedione and PPAR GAMMA agonist that is used in the treatment of TYPE 2 DIABETES MELLITUS.
pioglitazone : A member of the class of thiazolidenediones that is 1,3-thiazolidine-2,4-dione substituted by a benzyl group at position 5 which in turn is substituted by a 2-(5-ethylpyridin-2-yl)ethoxy group at position 4 of the phenyl ring. It exhibits hypoglycemic activity.

Body Weight: The mass or quantity of heaviness of an individual. It is expressed by units of pounds or kilograms.

Research Excerpts

Excerpt	Relevance	Reference
"The effects of dapagliflozin (DAP) and pioglitazone (PIO) on body weight and glycaemic control were compared in patients with type 2 diabetes mellitus."	9.30	Effect of switching from pioglitazone to the sodium glucose co-transporter-2 inhibitor dapagliflozin on body weight and metabolism-related factors in patients with type 2 diabetes mellitus: An open-label, prospective, randomized, parallel-group comparison ( Aoki, S; Atsumi, T; Cho, KY; Kurihara, Y; Manda, N; Miya, A; Miyoshi, H; Nakamura, A; Omori, K; Takase, T, 2019)
" After 12 weeks' treatment, the pioglitazone group showed a highly significant reduction in body weight (83±10."	9.24	Pioglitazone attenuates cardiometabolic risk factors in non-diabetic patients with dyslipidemia. ( Akhtar, L; Hussain, M; Shad, MN, 2017)
"To determine the effects of low-dose pioglitazone on plasma adipocyte-derived cytokines, high-sensitivity C-reactive protein (hs-CRP), and components of the metabolic syndrome in adults with the metabolic syndrome without diabetes mellitus."	9.22	Pharmacodynamic Effects of Low-Dose Pioglitazone in Patients with the Metabolic Syndrome without Diabetes Mellitus. ( Aquilante, CL; Beitelshees, AL; Bredbeck, B; Deininger, KM; Kosmiski, LA; Predhomme, J; Prigeon, R; Sidhom, MS; Vu, A, 2016)
"This study examined the effects of pioglitazone on body weight and bone mineral density (BMD) prospectively in patients with impaired glucose tolerance as pioglitazone (TZD) increases body weight and body fat in diabetic patients and increases the risk of bone fractures."	9.17	Effect of pioglitazone on body composition and bone density in subjects with prediabetes in the ACT NOW trial. ( Banerji, MA; Bray, GA; Buchanan, TA; Clement, SC; DeFronzo, RA; Henry, RR; Kitabchi, AE; Mudaliar, S; Musi, N; Ratner, RE; Reaven, PD; Schwenke, DC; Smith, SR; Stentz, FB; Tripathy, D, 2013)
"Pioglitazone ameliorates insulin resistance, but has an adverse effect of oedema that may result in subsequent heart failure, especially in diabetic patients with coronary artery disease."	9.17	Effects of low-dose pioglitazone on glucose control, lipid profiles, renin-angiotensin-aldosterone system and natriuretic peptides in diabetic patients with coronary artery disease. ( Dohi, Y; Ishibashi, K; Iwasaki, T; Kihara, Y; Kurisu, S; Mitsuba, N; Nishioka, K, 2013)
"We designed a study, involving 52 patients of 19-36 years of age, to test the pioglitazone in women with polycystic ovary syndrome."	9.16	Pioglitazone reduces central obesity in polycystic ovary syndrome women. ( Asadipooya, K; Kalantar-Hormozi, M; Nabipour, I, 2012)
"In patients with type 2 diabetes inadequately controlled on pioglitazone, the addition of dapagliflozin further reduced HbA(1c) levels and mitigated the pioglitazone-related weight gain without increasing hypoglycemia risk."	9.16	Effects of dapagliflozin, an SGLT2 inhibitor, on HbA(1c), body weight, and hypoglycemia risk in patients with type 2 diabetes inadequately controlled on pioglitazone monotherapy. ( List, JF; Rosenstock, J; Salsali, A; Vico, M; Wei, L, 2012)
"To evaluate the effects of intensive insulin therapy alone and with added pioglitazone on body weight, fat distribution, lean body mass (LBM) and liver fat in type 2 diabetic patients."	9.15	Effects of intensive insulin therapy alone and in combination with pioglitazone on body weight, composition, distribution and liver fat content in patients with type 2 diabetes. ( Andre, M; Aroda, V; Burke, P; Chang, AR; Henry, RR; Mudaliar, S; Shah, PK, 2011)
" Pioglitazone treatment (n = 10) reduced hepatic fat as assessed by magnetic resonance spectroscopy, despite a significant increase in body weight (Δ = 3."	9.15	Exenatide decreases hepatic fibroblast growth factor 21 resistance in non-alcoholic fatty liver disease in a mouse model of obesity and in a randomised controlled trial. ( Bajaj, M; Chan, L; Gonzalez, EV; Gutierrez, A; Jogi, M; Krishnamurthy, R; Muthupillai, R; Samson, SL; Sathyanarayana, P, 2011)
"The aim of this study was to investigate the effects of pioglitazone or metformin on bone mass and atherosclerosis in patients with type 2 diabetes."	9.14	Baseline atherosclerosis parameter could assess the risk of bone loss during pioglitazone treatment in type 2 diabetes mellitus. ( Kanazawa, I; Kurioka, S; Sugimoto, T; Yamaguchi, T; Yamamoto, M; Yamauchi, M; Yano, S, 2010)
"The purpose of this research was to evaluate the short-term effects of pioglitazone (PIO) on high-density lipoprotein cholesterol (HDL-C) and other metabolic parameters in nondiabetic patients with metabolic syndrome (MetSyn)."	9.12	Effects of pioglitazone on lipoproteins, inflammatory markers, and adipokines in nondiabetic patients with metabolic syndrome. ( Bloedon, LT; Chittams, J; Duffy, D; Rader, DJ; Reilly, MP; Samaha, FF; Soffer, D; Szapary, PO; Wolfe, ML, 2006)
"Our study aimed to investigate the effect of pioglitazone (PIO) on the obesity-associated metabolic effects and whether this effect is associated with modulation of catechol O-methyl transferase (COMT) expression in the high fat diet (HFD) induced obese rats."	7.96	Pioglitazone ameliorates high fat diet-induced hypertension and induces catechol o-methyl transferase expression in rats. ( Abd Elaziz, AI; Abulsoud, AI; El-Shafey, M; Elsadek, BEM; Hegazy, M; Salama, SA, 2020)
"The purpose of this work was to compare the influences of sulforaphane (SFN) to those of the standard insulin sensitizer pioglitazone (PIO) on high fructose diet (HFrD)-induced insulin resistance, dyslipidemia, hepatosteatosis, and vascular dysfunction in rats."	7.91	Comparison of the effects of sulforaphane and pioglitazone on insulin resistance and associated dyslipidemia, hepatosteatosis, and endothelial dysfunction in fructose-fed rats. ( Gameil, NM; Shawky, NM; Shehatou, GSG; Suddek, GM, 2019)
"Neither KD treatment nor pioglitazone alone or in combination affected clonic seizures."	7.85	Synergistic protection against acute flurothyl-induced seizures by adjuvant treatment of the ketogenic diet with the type 2 diabetes drug pioglitazone. ( Matthews, SA; Simeone, KA; Simeone, TA, 2017)
" In a post hoc meta-analysis of combined data from the 2 studies (n = 124), there was considerable overlapping in AUC(infinity) values between gender and race (Caucasians, Blacks, and Hispanics), making neither gender- nor racial-based dosing of pioglitazone or metformin necessary."	7.82	Oral antidiabetic drugs: bioavailability assessment of fixed-dose combination tablets of pioglitazone and metformin. Effect of body weight, gender, and race on systemic exposures of each drug. ( Bradford, D; Cao, C; Karim, A; Laurent, A; Schwartz, L; Slater, M; Zhao, Z, 2007)
"This study was carried out to highlight the role of PPARγ in the paraquat (PQ)-induced pulmonary fibrosis."	7.79	Antifibrotic effect of atorvastatin on paraquat-induced pulmonary fibrosis: role of PPARγ receptors. ( Khoramjouy, M; Malekinejad, H; Mehrabi, M; Rezaei-Golmisheh, A, 2013)
" We investigated the effect of cafeteria diet and pioglitazone on body weight, insulin resistance, and adiponectin/ghrelin levels in an experimental study on male Wistar rats."	7.78	A study on the short-term effect of cafeteria diet and pioglitazone on insulin resistance and serum levels of adiponectin and ghrelin. ( Bazzo, ML; Colombo, G; Colombo, MD; d'Acampora, AJ; Nogueira, CL; Schiavon, LL, 2012)
" Liraglutide leading to improve not only glycaemic control but also liver inflammation in non-alcoholic fatty liver disease (NAFLD) patients."	7.78	The effectiveness of liraglutide in nonalcoholic fatty liver disease patients with type 2 diabetes mellitus compared to sitagliptin and pioglitazone. ( Isogawa, A; Iwamoto, M; Koike, K; Ohki, T; Ohsugi, M; Omata, M; Tagawa, K; Toda, N; Yoshida, H, 2012)
"Pioglitazone improves insulin resistance in diabetics but often causes body weight gain."	7.77	Pioglitazone-induced body weight gain is prevented by combined administration with the lipoprotein lipase activator NO-1886. ( Habu, S; Kusunoki, M; Miyata, T; Mori, Y; Morishita, M; Nakamura, A; Nakamura, T; Nakaya, Y; Sato, D; Tsutsumi, K; Yonemoto, T, 2011)
"The aim of this study was to evaluate the efficacy of pioglitazone on metabolic parameters in drug-naïve Japanese type 2 diabetic patients with (Diabetes Mellitus Metabolic Syndrome [DMMS] group, n = 36) and without (Diabetes Mellitus non-Metabolic Sundrome [DMNMS] group, n = 36) metabolic syndrome."	7.76	Differential effects of pioglitazone on metabolic parameters in newly diagnosed, drug-naïve Japanese patients with type 2 diabetes with or without metabolic syndrome. ( Kutoh, E, 2010)
"In 6- and 10-week-old obesity-prone (fa/fa) Zucker diabetic fatty (ZDF) rats, effects of prevention and intervention therapies, respectively, were compared between PPARalpha/gamma agonist, ragaglitazar (RAGA) and separate PPARgamma and alpha agonists, pioglitazone (PIO) and bezafibrate (BF)."	7.73	The dual PPARalpha/gamma agonist, ragaglitazar, improves insulin sensitivity and metabolic profile equally with pioglitazone in diabetic and dietary obese ZDF rats. ( Brand, CL; Pickavance, LC; Wassermann, K; Wilding, JP, 2005)
"The data suggest that treatment with pioglitazone improves insulin sensitivity in low-dose STZ and high sucrose-fat diet induced obese rats."	7.73	Pioglitazone can ameliorate insulin resistance in low-dose streptozotocin and high sucrose-fat diet induced obese rats. ( Chen, YT; Ding, SY; Liu, Q; Shen, ZF; Sun, SJ; Xie, MZ, 2005)
"The present study investigates the effect of pioglitazone treatment on blood pressure, vascular reactivity and antioxidant enzymes in L-NAME induced hypertension in normal and STZ-diabetic rats."	7.73	Effect of pioglitazone on L-NAME induced hypertension in diabetic rats. ( Balaraman, R; Majithiya, JB; Parmar, AN; Trivedi, CJ, 2005)
"We measured plasma oleate concentration and flux ([(3)H]oleate), glucose kinetics ([6-(2)H(2)]glucose) and substrate oxidation (indirect calorimetry) before and after pioglitazone (30 mg/day for approximately 20 weeks) in 20 non-diabetic adults with upper body obesity."	7.73	Pioglitazone increases non-esterified fatty acid clearance in upper body obesity. ( Jensen, MD; Shadid, S, 2006)
" We investigated the effect of pioglitazone, a peroxisome proliferator-activated receptor-gamma ligand, on dextran sulfate sodium-induced colonic mucosal injury and inflammation in mice."	7.71	Pioglitazone, a PPAR-gamma ligand, provides protection from dextran sulfate sodium-induced colitis in mice in association with inhibition of the NF-kappaB-cytokine cascade. ( Handa, O; Ichikawa, H; Naito, Y; Takagi, T; Tomatsuri, N; Yoshida, N; Yoshikawa, T, 2002)
"HCl and metformin on diabetes and obesity were investigated in Wistar fatty rats, which are hyperglycaemic and hypertriglyceridaemic and have higher plasma levels of total ketone bodies than lean rats."	7.71	Effects of combined pioglitazone and metformin on diabetes and obesity in Wistar fatty rats. ( Ikeda, H; Odaka, H; Sugiyama, Y; Suzuki, M; Suzuki, N, 2002)
"We examined the effect of pioglitazone on abdominal fat distribution to elucidate the mechanisms via which pioglitazone improves insulin resistance in patients with type 2 diabetes mellitus."	7.71	Effect of pioglitazone on abdominal fat distribution and insulin sensitivity in type 2 diabetic patients. ( Cusi, K; DeFronzo, RA; Hardies, J; Mahankali, A; Mahankali, S; Mandarino, LJ; Matsuda, M; Miyazaki, Y, 2002)
"Effects of pioglitazone (5-[4-[2-(5-etyl-2-pyridyl)ethoxy] benzyl]-2,4-thiazolidinedione, AD-4833, also known as U-72, 107E) on peripheral and hepatic insulin resistance were examined using genetically obese-hyperglycemic rats, Wistar fatty."	7.68	Effects of pioglitazone on hepatic and peripheral insulin resistance in Wistar fatty rats. ( Ikeda, H; Shimura, Y; Sugiyama, Y, 1990)
"Isohumulone treatment did not result in significant body weight gain, although pioglitazone treatment did increase body weight (10."	6.71	Isohumulones, bitter acids derived from hops, activate both peroxisome proliferator-activated receptor alpha and gamma and reduce insulin resistance. ( Ezaki, O; Fujiwara, D; Ikeshima, E; Kanaya, T; Kondo, K; Odai, H; Oikawa, S; Shiraki, M; Tsuboyama-Kasaoka, N; Yajima, H, 2004)
"Pioglitazone treatment did not influence body weight or ovarian weight in either group."	5.48	Pioglitazone is effective for multiple phenotyepes of the Zucker fa/fa rat with polycystc ovary morphology and insulin resistance. ( Baba, T; Endo, T; Honnma, H; Ikeda, K; Kiya, T; Kuno, Y; Morishita, M; Saito, T, 2018)
"In LNCaP, a human androgen-dependent prostate cancer cell line, PGZ also inhibited cyclin D1 expression and the activation of both p38 MAPK and NFκB."	5.43	Pioglitazone, a Peroxisome Proliferator-Activated Receptor γ Agonist, Suppresses Rat Prostate Carcinogenesis. ( Kato, H; Kobayashi, M; Kuno, T; Mori, Y; Nagano, A; Nagayasu, Y; Naiki-Ito, A; Suzuki, S; Takahashi, S, 2016)
"Treatment with pioglitazone or nicorandil either alone or in combination successfully ameliorated the deleterious effects of HFD on the all previous parameters."	5.42	Ameliorative effect of nicorandil on high fat diet induced non-alcoholic fatty liver disease in rats. ( Elshazly, SM, 2015)
"Rats treated with boswellic acids (125 or 250 mg/kg) or pioglitazone showed improved insulin sensitivity and a reduction in liver index, activities of liver enzymes, serum TNF-α and IL-6 as well as hepatic iNOS expression and HNE formation compared to HFD group."	5.42	Protective effect of boswellic acids versus pioglitazone in a rat model of diet-induced non-alcoholic fatty liver disease: influence on insulin resistance and energy expenditure. ( Abdelaziz, EZ; Barakat, BM; Bilasy, SE; Farag, NE; Fawzy, MS; Zaitone, SA, 2015)
"Cachexia is a multifactorial syndrome characterized by profound involuntary weight loss, fat depletion, skeletal muscle wasting, and asthenia; all symptoms are not entirely attributable to inadequate nutritional intake."	5.42	Pioglitazone treatment increases survival and prevents body weight loss in tumor-bearing animals: possible anti-cachectic effect. ( Andreotti, S; Batista, ML; Beluzi, M; Farmer, SR; Franco, FO; Henriques, FS; Knobl, P; Lima, FB; Neves, RX; Peres, SB; Santos, KB; Seelaender, M; Sertié, RA; Shida, CS, 2015)
"Pioglitazone has been demonstrated to have beneficial effects on cardiovascular outcomes."	5.38	Pioglitazone attenuates cardiac fibrosis and hypertrophy in a rat model of diabetic nephropathy. ( Asker, ME; Elrashidy, RA; Mohamed, HE, 2012)
"Emodin is an active herbal component traditionally used in China for treating a variety of diseases."	5.38	Emodin protects against high-fat diet-induced obesity via regulation of AMP-activated protein kinase pathways in white adipose tissue. ( Chang, CJ; Liou, SS; Liu, IM; Lu, HJ; Tzeng, TF, 2012)
"Telmisartan is an angiotensin II receptor blocker with peroxisome proliferator-activated receptor-gamma agonistic properties."	5.36	Neuroendocrine characterization and anorexigenic effects of telmisartan in diet- and glitazone-induced weight gain. ( Aubert, G; Burnier, M; Dulloo, A; Mazzolai, L; Perregaux, C; Pralong, F; Zanchi, A, 2010)
"Metformin treatment also improved hyperleptinemia, whereas pioglitazone was ineffective."	5.36	Metformin reduces body weight gain and improves glucose intolerance in high-fat diet-fed C57BL/6J mice. ( Hirasawa, Y; Ito, M; Kyuki, K; Matsui, Y; Sugiura, T; Toyoshi, T, 2010)
"Non-alcoholic steatohepatitis (NASH) may progress to liver cirrhosis, and NASH patients with liver cirrhosis have a risk of development of hepatocellular carcinoma."	5.32	Pioglitazone prevents hepatic steatosis, fibrosis, and enzyme-altered lesions in rat liver cirrhosis induced by a choline-deficient L-amino acid-defined diet. ( Kawaguchi, K; Okita, K; Omori, K; Sakaida, I; Takami, T; Tsuchiya, M, 2004)
"Treatment with pioglitazone (10 and 30 mg/kg p."	5.32	Reversal of glucose intolerance by by pioglitazone in high fat diet-fed rats. ( Kaul, CL; Patole, PS; Ramarao, P; Srinivasan, K, 2004)
"The effects of dapagliflozin (DAP) and pioglitazone (PIO) on body weight and glycaemic control were compared in patients with type 2 diabetes mellitus."	5.30	Effect of switching from pioglitazone to the sodium glucose co-transporter-2 inhibitor dapagliflozin on body weight and metabolism-related factors in patients with type 2 diabetes mellitus: An open-label, prospective, randomized, parallel-group comparison ( Aoki, S; Atsumi, T; Cho, KY; Kurihara, Y; Manda, N; Miya, A; Miyoshi, H; Nakamura, A; Omori, K; Takase, T, 2019)
"Glyburide did not increase basal or insulin-stimulated DNA synthesis."	5.30	Pioglitazone: in vitro effects on rat hepatoma cells and in vivo liver hypertrophy in KKAy mice. ( Diani, A; Messina, JL; Murray, FT; Sangani, GA; Wachowski, MB; Weinstock, RS, 1997)
"Insulin sensitivity was increased by pioglitazone hydrochloride (P = 0."	5.29	Pioglitazone increases insulin sensitivity, reduces blood glucose, insulin, and lipid levels, and lowers blood pressure, in obese, insulin-resistant rhesus monkeys. ( Baum, ST; Bergman, RN; Elson, DF; Kemnitz, JW; Meglasson, MD; Roecker, EB, 1994)
" After 12 weeks' treatment, the pioglitazone group showed a highly significant reduction in body weight (83±10."	5.24	Pioglitazone attenuates cardiometabolic risk factors in non-diabetic patients with dyslipidemia. ( Akhtar, L; Hussain, M; Shad, MN, 2017)
"To determine the effects of low-dose pioglitazone on plasma adipocyte-derived cytokines, high-sensitivity C-reactive protein (hs-CRP), and components of the metabolic syndrome in adults with the metabolic syndrome without diabetes mellitus."	5.22	Pharmacodynamic Effects of Low-Dose Pioglitazone in Patients with the Metabolic Syndrome without Diabetes Mellitus. ( Aquilante, CL; Beitelshees, AL; Bredbeck, B; Deininger, KM; Kosmiski, LA; Predhomme, J; Prigeon, R; Sidhom, MS; Vu, A, 2016)
" Patients treated with exenatide lost body weight remarkably (-4."	5.20	Effect of exenatide, insulin and pioglitazone on bone metabolism in patients with newly diagnosed type 2 diabetes. ( Li, R; Luo, S; Tong, G; Weng, J; Xu, H; Xu, W; Zeng, L; Zhu, D, 2015)
"This study examined the effects of pioglitazone on body weight and bone mineral density (BMD) prospectively in patients with impaired glucose tolerance as pioglitazone (TZD) increases body weight and body fat in diabetic patients and increases the risk of bone fractures."	5.17	Effect of pioglitazone on body composition and bone density in subjects with prediabetes in the ACT NOW trial. ( Banerji, MA; Bray, GA; Buchanan, TA; Clement, SC; DeFronzo, RA; Henry, RR; Kitabchi, AE; Mudaliar, S; Musi, N; Ratner, RE; Reaven, PD; Schwenke, DC; Smith, SR; Stentz, FB; Tripathy, D, 2013)
"Pioglitazone ameliorates insulin resistance, but has an adverse effect of oedema that may result in subsequent heart failure, especially in diabetic patients with coronary artery disease."	5.17	Effects of low-dose pioglitazone on glucose control, lipid profiles, renin-angiotensin-aldosterone system and natriuretic peptides in diabetic patients with coronary artery disease. ( Dohi, Y; Ishibashi, K; Iwasaki, T; Kihara, Y; Kurisu, S; Mitsuba, N; Nishioka, K, 2013)
"We designed a study, involving 52 patients of 19-36 years of age, to test the pioglitazone in women with polycystic ovary syndrome."	5.16	Pioglitazone reduces central obesity in polycystic ovary syndrome women. ( Asadipooya, K; Kalantar-Hormozi, M; Nabipour, I, 2012)
"To assess the association of weight and weight change with mortality and non-fatal cardiovascular outcomes (hospitalisation, myocardial infarction and stroke) in T2DM patients with cardiovascular co-morbidity and the effect of pioglitazone-induced weight change on mortality."	5.16	Inverse relation of body weight and weight change with mortality and morbidity in patients with type 2 diabetes and cardiovascular co-morbidity: an analysis of the PROactive study population. ( Anker, SD; Cairns, R; Clark, AL; Doehner, W; Dormandy, JA; Erdmann, E; Ferrannini, E, 2012)
"In patients with type 2 diabetes inadequately controlled on pioglitazone, the addition of dapagliflozin further reduced HbA(1c) levels and mitigated the pioglitazone-related weight gain without increasing hypoglycemia risk."	5.16	Effects of dapagliflozin, an SGLT2 inhibitor, on HbA(1c), body weight, and hypoglycemia risk in patients with type 2 diabetes inadequately controlled on pioglitazone monotherapy. ( List, JF; Rosenstock, J; Salsali, A; Vico, M; Wei, L, 2012)
"In T2DM, low dose pioglitazone (15 mg/day) increases 15-epi-LXA(4) and adiponectin levels in the absence of significant changes in body weight."	5.16	The effect of pioglitazone treatment on 15-epi-lipoxin A4 levels in patients with type 2 diabetes. ( Bajaj, M; Birnbaum, Y; Gutierrez, AD; Konduru, S; Sathyanarayana, P; Ye, Y, 2012)
"To evaluate the effects of intensive insulin therapy alone and with added pioglitazone on body weight, fat distribution, lean body mass (LBM) and liver fat in type 2 diabetic patients."	5.15	Effects of intensive insulin therapy alone and in combination with pioglitazone on body weight, composition, distribution and liver fat content in patients with type 2 diabetes. ( Andre, M; Aroda, V; Burke, P; Chang, AR; Henry, RR; Mudaliar, S; Shah, PK, 2011)
" Pioglitazone treatment (n = 10) reduced hepatic fat as assessed by magnetic resonance spectroscopy, despite a significant increase in body weight (Δ = 3."	5.15	Exenatide decreases hepatic fibroblast growth factor 21 resistance in non-alcoholic fatty liver disease in a mouse model of obesity and in a randomised controlled trial. ( Bajaj, M; Chan, L; Gonzalez, EV; Gutierrez, A; Jogi, M; Krishnamurthy, R; Muthupillai, R; Samson, SL; Sathyanarayana, P, 2011)
" Vildagliptin provided additional HbA(1c) lowering to that achieved with metformin alone and comparable to that achieved with pioglitazone, with only pioglitazone causing weight gain."	5.14	Comparison of vildagliptin and pioglitazone in patients with type 2 diabetes inadequately controlled with metformin. ( Bolli, G; Colin, L; Dotta, F; Goodman, M; Minic, B, 2009)
"The aim of the study was to compare the effects of the addition of sitagliptin or metformin to pioglitazone monotherapy in poorly controlled type 2 diabetes mellitus patients on body weight, glycemic control, beta-cell function, insulin resistance, and inflammatory state parameters."	5.14	Effects of sitagliptin or metformin added to pioglitazone monotherapy in poorly controlled type 2 diabetes mellitus patients. ( Ciccarelli, L; Cicero, AF; D'Angelo, A; Derosa, G; Ferrari, I; Franzetti, IG; Gadaleta, G; Maffioli, P; Piccinni, MN; Querci, F; Ragonesi, PD; Salvadeo, SA, 2010)
"The aim of this study was to investigate the effects of pioglitazone or metformin on bone mass and atherosclerosis in patients with type 2 diabetes."	5.14	Baseline atherosclerosis parameter could assess the risk of bone loss during pioglitazone treatment in type 2 diabetes mellitus. ( Kanazawa, I; Kurioka, S; Sugimoto, T; Yamaguchi, T; Yamamoto, M; Yamauchi, M; Yano, S, 2010)
"Pioglitazone was associated with a rapid increase in body weight and an increase in diurnal proximal sodium reabsorption, without any change in renal haemodynamics or in the modulation of the renin-angiotensin aldosterone system to changes in salt intake."	5.14	Effects of the peroxisome proliferator-activated receptor (PPAR)-gamma agonist pioglitazone on renal and hormonal responses to salt in diabetic and hypertensive individuals. ( Burnier, M; Deleaval, P; Jornayvaz, FR; Maillard, M; Nussberger, J; Pechere-Bertschi, A; Vinciguerra, M; Zanchi, A, 2010)
"The aim of the study was to compare the effects of vildagliptin added to pioglitazone or glimepiride on metabolic and insulin resistance related-indices in poorly controlled type 2 diabetic patients (T2DM)."	5.14	Effects of one year treatment of vildagliptin added to pioglitazone or glimepiride in poorly controlled type 2 diabetic patients. ( Ciccarelli, L; D'Angelo, A; Derosa, G; Ferrari, I; Franzetti, IG; Gadaleta, G; Maffioli, P; Mereu, R; Piccinni, MN; Querci, F; Ragonesi, PD; Salvadeo, SA, 2010)
"Effects of metformin and pioglitazone on body weight are clearly different."	5.13	Metformin, but not pioglitazone, decreases postchallenge plasma ghrelin levels in type 2 diabetic patients: a possible role in weight stability? ( Horie, H; Ishibashi, S; Kusaka, I; Nagasaka, S, 2008)
"The purpose of this research was to evaluate the short-term effects of pioglitazone (PIO) on high-density lipoprotein cholesterol (HDL-C) and other metabolic parameters in nondiabetic patients with metabolic syndrome (MetSyn)."	5.12	Effects of pioglitazone on lipoproteins, inflammatory markers, and adipokines in nondiabetic patients with metabolic syndrome. ( Bloedon, LT; Chittams, J; Duffy, D; Rader, DJ; Reilly, MP; Samaha, FF; Soffer, D; Szapary, PO; Wolfe, ML, 2006)
"The Pioglitazone In Prevention Of Diabetes (PIPOD) study was conducted to evaluate beta-cell function, insulin resistance, and the incidence of diabetes during treatment with pioglitazone in Hispanic women with prior gestational diabetes who had completed participation in the Troglitazone In Prevention Of Diabetes (TRIPOD) study."	5.12	Effect of pioglitazone on pancreatic beta-cell function and diabetes risk in Hispanic women with prior gestational diabetes. ( Buchanan, TA; Goico, J; Kawakubo, M; Kjos, SL; Marroquin, A; Ochoa, C; Peters, RK; Xiang, AH, 2006)
" The traditional approach involves: i) metformin, acting mainly on fasting blood glucose; ii) sulphonylureas, that have shown a number of drawbacks, including the high risk of hypoglycemia; iii) pioglitazone, with a substantial effect on fasting and postprandial glucose and a low risk of hypoglycaemia; iv) insulin, that can be utilized with the basal or prandial approach."	4.89	What are the preferred strategies for control of glycaemic variability in patients with type 2 diabetes mellitus? ( Marangoni, A; Zenari, L, 2013)
"The antidiabetic compound pioglitazone, an activator of the intracellular peroxisome proliferator-activated receptor-gamma, and decreases metabolic and vascular insulin resistance."	4.83	Pioglitazone: an antidiabetic drug with cardiovascular therapeutic effects. ( Forst, T; Pfützner, A; Schneider, CA, 2006)
"The combination of pioglitazone and α-lipoic acid has a significantly improving effect on BMI, body weight, oxidative stress levels, lipid metabolism, and menstrual status."	4.31	Beneficial effects of pioglitazone and α-lipoic acid in patients with polycystic ovaries syndrome. ( Hu, H; Liu, YY; Pei, Y; Sun, M; Wang, B; Wang, ZL; Zheng, J; Zhou, TT, 2023)
"Our study aimed to investigate the effect of pioglitazone (PIO) on the obesity-associated metabolic effects and whether this effect is associated with modulation of catechol O-methyl transferase (COMT) expression in the high fat diet (HFD) induced obese rats."	3.96	Pioglitazone ameliorates high fat diet-induced hypertension and induces catechol o-methyl transferase expression in rats. ( Abd Elaziz, AI; Abulsoud, AI; El-Shafey, M; Elsadek, BEM; Hegazy, M; Salama, SA, 2020)
"The purpose of this work was to compare the influences of sulforaphane (SFN) to those of the standard insulin sensitizer pioglitazone (PIO) on high fructose diet (HFrD)-induced insulin resistance, dyslipidemia, hepatosteatosis, and vascular dysfunction in rats."	3.91	Comparison of the effects of sulforaphane and pioglitazone on insulin resistance and associated dyslipidemia, hepatosteatosis, and endothelial dysfunction in fructose-fed rats. ( Gameil, NM; Shawky, NM; Shehatou, GSG; Suddek, GM, 2019)
"To evaluate the effect of metformin and pioglitazone on leutinizing hormone and follicle stimulating hormone receptor mRNA expression, hyperandrogenism and insulin resistance in high fat diet induced and letrozole induced PCOS in rats."	3.88	Insulin Sensitizers Modulate GnRH Receptor Expression in PCOS Rats. ( Patel, R; Shah, G, 2018)
"Neither KD treatment nor pioglitazone alone or in combination affected clonic seizures."	3.85	Synergistic protection against acute flurothyl-induced seizures by adjuvant treatment of the ketogenic diet with the type 2 diabetes drug pioglitazone. ( Matthews, SA; Simeone, KA; Simeone, TA, 2017)
"Our study indicates that combination therapy with canagliflozin and pioglitazone improves insulin sensitivity partly by preventing glucotoxicity and, at least partly, by attenuating pioglitazone-induced body weight gain in two different obese diabetic animal models."	3.81	Beneficial effects of canagliflozin in combination with pioglitazone on insulin sensitivity in rodent models of obese type 2 diabetes. ( Arakawa, K; Horai, Y; Kuriyama, C; Nakayama, K; Senbonmatsu, T; Shiotani, M; Taniuchi, N; Ueta, K; Watanabe, Y, 2015)
"Pioglitazone treatment significantly decreased serum RBP4 levels in obese rats, which was correlated with reduced body weight and increased insulin sensitivity."	3.81	Pioglitazone lowers serum retinol binding protein 4 by suppressing its expression in adipose tissue of obese rats. ( Han, J; Jia, W; Liu, X; Wei, L; Xiao, Y; Zhang, J; Zhu, C, 2015)
" A range of parameters was evaluated including body weight development, plasma levels of total cholesterol, triglycerides (TG), low-density-lipoprotein cholesterol, high-density lipoprotein cholesterol (HDL-C), adiponectin, leptin, glucose, insulin, interleukin-6 (IL-6), atherogenic index (AI) and the coronary risk index (CRI)."	3.80	Ficus carica leaf extract modulates the lipid profile of rats fed with a high-fat diet through an increase of HDL-C. ( Benedek, B; Bonnländer, B; Butterweck, V; Joerin, L; Kauschka, M; Pischel, I, 2014)
"Peroxisome proliferator-activated receptor-γ (PPARγ) agonists like pioglitazone (PGZ) are effective antidiabetic drugs, but they induce fluid retention and body weight (BW) gain."	3.80	Dipeptidyl peptidase IV inhibitor lowers PPARγ agonist-induced body weight gain by affecting food intake, fat mass, and beige/brown fat but not fluid retention. ( Czogalla, J; Eguchi, A; Feldstein, AE; Fu, Y; Gerasimova, M; Kuczkowski, A; Masuda, T; Rose, MA; Scadeng, M; Vallon, V, 2014)
"Administration of rutin (50 and 100 mg/kg) and pioglitazone (10 mg/kg) orally for 3 weeks treatment significantly improved body weight, reduced plasma glucose and glycosylated hemoglobin, pro-inflammatory cytokines (IL-6 and TNF-alpha), restored the depleted liver antioxidant status and serum lipid profile in high fat diet + streptozotocin induced type 2 diabetic rats."	3.80	Anti-hyperglycemic activity of rutin in streptozotocin-induced diabetic rats: an effect mediated through cytokines, antioxidants and lipid biomarkers. ( Ansari, AA; Naik, SR; Niture, NT, 2014)
" Administration of DAGA (200 mg/kg) reduced SBP and significantly improved the FPG and HOMA-IR (homeostatis model assessment-insulin resistance) with modest improvement in lipid profile without decrease in body weight similar to pioglitazone."	3.79	Effect of a deacyl gymnemic acid on glucose homeostasis & metabolic parameters in a rat model of metabolic syndrome. ( Bhansali, S; Malhotra, S; Pandhi, P; Shafiq, N; Sharma, S; Singh, AP; Singh, I; Singh, PK, 2013)
"Telmisartan acts beneficially against diabetes-induced inflammation and improves insulin resistance in pre-diabetes OLETF rats fed with HFD."	3.79	Angiotensin II receptor blocker telmisartan prevents new-onset diabetes in pre-diabetes OLETF rats on a high-fat diet: evidence of anti-diabetes action. ( Li, LY; Luo, R; Sun, LT; Tian, FS; Xiong, HL; Zhao, ZQ; Zheng, XL, 2013)
"This study was carried out to highlight the role of PPARγ in the paraquat (PQ)-induced pulmonary fibrosis."	3.79	Antifibrotic effect of atorvastatin on paraquat-induced pulmonary fibrosis: role of PPARγ receptors. ( Khoramjouy, M; Malekinejad, H; Mehrabi, M; Rezaei-Golmisheh, A, 2013)
" Herein, we demonstrate in mice that rosiglitazone (RGZ), a PPARγ ligand, increases body weight and abdominal fat pad fluid content and reduces hematocrit."	3.78	Peroxisome proliferator-activated receptor-γ agonists repress epithelial sodium channel expression in the kidney. ( Borsting, E; Cheng, VP; Cunard, R; Glass, CK; Vallon, V, 2012)
" We investigated the effect of cafeteria diet and pioglitazone on body weight, insulin resistance, and adiponectin/ghrelin levels in an experimental study on male Wistar rats."	3.78	A study on the short-term effect of cafeteria diet and pioglitazone on insulin resistance and serum levels of adiponectin and ghrelin. ( Bazzo, ML; Colombo, G; Colombo, MD; d'Acampora, AJ; Nogueira, CL; Schiavon, LL, 2012)
" In addition to measuring BW, circulating glucose level, and BP, the following procedures were also carried out: insulin challenge (insulin sensitivity), losartan challenge (renin-angiotensin system activity), Nw-nitro-L arginine-methyl ester hydrochloride (LNAME) challenge (nitric oxide [NO] system activity), and evaluation of serum angiotensin converting enzyme (ACE) activity."	3.78	Fraction SX of maitake mushroom favorably influences blood glucose levels and blood pressure in streptozotocin-induced diabetic rats. ( Bagchi, D; Echard, B; Fu, J; Kaylor, M; Perricone, NV; Preuss, HG; Zhuang, C, 2012)
" Liraglutide leading to improve not only glycaemic control but also liver inflammation in non-alcoholic fatty liver disease (NAFLD) patients."	3.78	The effectiveness of liraglutide in nonalcoholic fatty liver disease patients with type 2 diabetes mellitus compared to sitagliptin and pioglitazone. ( Isogawa, A; Iwamoto, M; Koike, K; Ohki, T; Ohsugi, M; Omata, M; Tagawa, K; Toda, N; Yoshida, H, 2012)
"Pioglitazone improves insulin resistance in diabetics but often causes body weight gain."	3.77	Pioglitazone-induced body weight gain is prevented by combined administration with the lipoprotein lipase activator NO-1886. ( Habu, S; Kusunoki, M; Miyata, T; Mori, Y; Morishita, M; Nakamura, A; Nakamura, T; Nakaya, Y; Sato, D; Tsutsumi, K; Yonemoto, T, 2011)
" The aim of this study was to investigate the relationship between accelerated atherosclerosis (AS) and the balance of regulatory/effector T cells (Treg/Teff) in uremic apolipoprotein E knockout (apoE-/-) mice, and the effect of pioglitazone on uremic AS and possible mechanisms."	3.77	Antiatherogenic effect of pioglitazone on uremic apolipoprotein E knockout mice by modulation of the balance of regulatory and effector T cells. ( Chen, T; Kishimoto, C; Liang, X; Liu, W; Liu, Y; Shen, Y; Tian, Y; Wang, L; Wu, Y; Xiao, Y; Yin, A; Yuan, Z; Zhao, Y, 2011)
"The present data indicated that a long-term high-fat diet could induce obesity metabolic syndrome in SD rats and finally lead to lower vaspin of sera and periepididymal fat, while pioglitazone and chronic calorie-control ingestion could enhance the production of vaspin."	3.76	Calorie control increased vaspin levels of serum and periepididymal adipose tissue in diet-induced obese rats in association with serum free fatty acid and tumor necrosis factor alpha. ( Lü, QH; Wang, LP; Wang, WP; Wang, YM; Zhou, XH, 2010)
" All rats were examined for body weight, serum and hepatic biochemical indices, content of malondialdehyde (MDA), activities of superoxide dismutase (SOD) and pathological changes in liver and pancreas, as well as protein tyrosine phosphatase 1B (PTP1B) expression in liver."	3.76	Antidiabetic effects of total flavonoids from Litsea Coreana leve on fat-fed, streptozotocin-induced type 2 diabetic rats. ( Cheng, WM; Hu, XY; Li, J; Lu, YX; Sun, YX; Wang, LY; Zhang, Q, 2010)
"The aim of this study was to evaluate the efficacy of pioglitazone on metabolic parameters in drug-naïve Japanese type 2 diabetic patients with (Diabetes Mellitus Metabolic Syndrome [DMMS] group, n = 36) and without (Diabetes Mellitus non-Metabolic Sundrome [DMNMS] group, n = 36) metabolic syndrome."	3.76	Differential effects of pioglitazone on metabolic parameters in newly diagnosed, drug-naïve Japanese patients with type 2 diabetes with or without metabolic syndrome. ( Kutoh, E, 2010)
" Here, in an animal model of obesity and insulin resistance, the metabolic response to cevoglitazar, a dual PPARalpha/gamma, was characterized using a combination of in vivo and ex vivo magnetic resonance methodologies and compared to treatment effects of fenofibrate, a PPARalpha agonist, and pioglitazone, a PPARgamma agonist."	3.75	Effects of cevoglitazar, a dual PPARalpha/gamma agonist, on ectopic fat deposition in fatty Zucker rats. ( Boettcher, BR; Gao, J; Gounarides, JS; Laurent, D, 2009)
"In 6- and 10-week-old obesity-prone (fa/fa) Zucker diabetic fatty (ZDF) rats, effects of prevention and intervention therapies, respectively, were compared between PPARalpha/gamma agonist, ragaglitazar (RAGA) and separate PPARgamma and alpha agonists, pioglitazone (PIO) and bezafibrate (BF)."	3.73	The dual PPARalpha/gamma agonist, ragaglitazar, improves insulin sensitivity and metabolic profile equally with pioglitazone in diabetic and dietary obese ZDF rats. ( Brand, CL; Pickavance, LC; Wassermann, K; Wilding, JP, 2005)
"The data suggest that treatment with pioglitazone improves insulin sensitivity in low-dose STZ and high sucrose-fat diet induced obese rats."	3.73	Pioglitazone can ameliorate insulin resistance in low-dose streptozotocin and high sucrose-fat diet induced obese rats. ( Chen, YT; Ding, SY; Liu, Q; Shen, ZF; Sun, SJ; Xie, MZ, 2005)
"The present study investigates the effect of pioglitazone treatment on blood pressure, vascular reactivity and antioxidant enzymes in L-NAME induced hypertension in normal and STZ-diabetic rats."	3.73	Effect of pioglitazone on L-NAME induced hypertension in diabetic rats. ( Balaraman, R; Majithiya, JB; Parmar, AN; Trivedi, CJ, 2005)
"We measured plasma oleate concentration and flux ([(3)H]oleate), glucose kinetics ([6-(2)H(2)]glucose) and substrate oxidation (indirect calorimetry) before and after pioglitazone (30 mg/day for approximately 20 weeks) in 20 non-diabetic adults with upper body obesity."	3.73	Pioglitazone increases non-esterified fatty acid clearance in upper body obesity. ( Jensen, MD; Shadid, S, 2006)
" Therefore, we examined the effect of pioglitazone, a PPARgamma agonist, on chronic left ventricular remodeling after experimental myocardial infarction (MI) in mice."	3.72	Peroxisome proliferator activated-receptor agonism and left ventricular remodeling in mice with chronic myocardial infarction. ( Bauersachs, J; Bayer, B; Ertl, G; Frantz, S; Galuppo, P; Hu, K; Schmidt, I; Strotmann, J; Widder, J; Witzel, CC, 2004)
" We investigated the effect of pioglitazone, a peroxisome proliferator-activated receptor-gamma ligand, on dextran sulfate sodium-induced colonic mucosal injury and inflammation in mice."	3.71	Pioglitazone, a PPAR-gamma ligand, provides protection from dextran sulfate sodium-induced colitis in mice in association with inhibition of the NF-kappaB-cytokine cascade. ( Handa, O; Ichikawa, H; Naito, Y; Takagi, T; Tomatsuri, N; Yoshida, N; Yoshikawa, T, 2002)
" In the present study, we examined the role of PPARgamma in angiotensin II (Ang II)-induced hypertrophy of neonatal rat cardiac myocytes and in pressure overload-induced cardiac hypertrophy of mice."	3.71	Peroxisome proliferator-activated receptor gamma plays a critical role in inhibition of cardiac hypertrophy in vitro and in vivo. ( Asakawa, M; Hasegawa, H; Kadowaki, T; Komuro, I; Kubota, N; Masuda, Y; Nagai, T; Saito, T; Takano, H; Uozumi, H, 2002)
" The body weight, daily food intake, plasma levels of fat, insulin, leptin and the wet weight of visceral fat were not influenced, but the levels of blood hemoglobin Alc and plasma tumor necrosis factor a were decreased by pioglitazone."	3.71	A peroxisome proliferator-activated receptor gamma agonist influenced daily profile of energy expenditure in genetically obese diabetic rats. ( Funakoshi, A; Ichikawa, M; Ichimaru, Y; Kanai, S; Kobayash, M; Miyasak, K; Ohta, M; Shimazoe, T; Watanabe, S; Yoshida, Y, 2002)
"HCl and metformin on diabetes and obesity were investigated in Wistar fatty rats, which are hyperglycaemic and hypertriglyceridaemic and have higher plasma levels of total ketone bodies than lean rats."	3.71	Effects of combined pioglitazone and metformin on diabetes and obesity in Wistar fatty rats. ( Ikeda, H; Odaka, H; Sugiyama, Y; Suzuki, M; Suzuki, N, 2002)
"We examined the effect of pioglitazone on abdominal fat distribution to elucidate the mechanisms via which pioglitazone improves insulin resistance in patients with type 2 diabetes mellitus."	3.71	Effect of pioglitazone on abdominal fat distribution and insulin sensitivity in type 2 diabetic patients. ( Cusi, K; DeFronzo, RA; Hardies, J; Mahankali, A; Mahankali, S; Mandarino, LJ; Matsuda, M; Miyazaki, Y, 2002)
" Pioglitazone, a thiazolidinedione derivative, sensitizes target tissues to insulin and decreases hyperglycemia and hyperinsulinemia in various insulin-resistant animals."	3.70	Pioglitazone attenuates basal and postprandial insulin concentrations and blood pressure in the spontaneously hypertensive rat. ( Gonzalez, R; Grinsell, JW; Lardinois, CK; Michaels, JR; Sare, JS; Starich, GH; Swislocki, A, 2000)
" Oral administration of pioglitazone (20 mg/kg twice daily or 40 mg/kg/day for 4 weeks), an agent known to ameliorate insulin sensitivity, significantly decreased plasma glucose levels during the treatment period."	3.69	KB-R7785, a novel matrix metalloproteinase inhibitor, exerts its antidiabetic effect by inhibiting tumor necrosis factor-alpha production. ( Morimoto, Y; Nishikawa, K; Ohashi, M, 1997)
" To address this problem, we have studied the in vivo effect of pioglitazone on glucose metabolism and gene expression in the adipose tissue of an animal model of obesity with insulin resistance, the obese Zucker (fa/fa) rat."	3.69	Pioglitazone induces in vivo adipocyte differentiation in the obese Zucker fa/fa rat. ( Auwerx, J; Berthault, MF; Doaré, L; Dugail, I; Ferré, P; Foufelle, F; Guerre-Millo, M; Hallakou, S; Kergoat, M; Morin, J, 1997)
"Effects of pioglitazone (5-[4-[2-(5-etyl-2-pyridyl)ethoxy] benzyl]-2,4-thiazolidinedione, AD-4833, also known as U-72, 107E) on peripheral and hepatic insulin resistance were examined using genetically obese-hyperglycemic rats, Wistar fatty."	3.68	Effects of pioglitazone on hepatic and peripheral insulin resistance in Wistar fatty rats. ( Ikeda, H; Shimura, Y; Sugiyama, Y, 1990)
"More likely, hemodynamic effects, specifically reduced blood pressure and decreased extracellular volume, are responsible for the reduction in CV mortality and heart failure hospitalization."	2.82	SGLT2 Inhibitors and Cardiovascular Risk: Lessons Learned From the EMPA-REG OUTCOME Study. ( Abdul-Ghani, M; Chilton, R; DeFronzo, RA; Del Prato, S, 2016)
"Pioglitazone was more effective than glibenclamide in improving inflammation and hepatic steatosis indices."	2.78	Ultrasonography modifications of visceral and subcutaneous adipose tissue after pioglitazone or glibenclamide therapy combined with rosuvastatin in type 2 diabetic patients not well controlled by metformin. ( D'Angelo, A; Derosa, G; Fogari, E; Maffioli, P; Perrone, T, 2013)
" Average increases in insulin dosage with exenatide and placebo were 13 U/d and 20 U/d."	2.76	Use of twice-daily exenatide in Basal insulin-treated patients with type 2 diabetes: a randomized, controlled trial. ( Bergenstal, RM; Buse, JB; Glass, LC; Heilmann, CR; Hoogwerf, BJ; Kwan, AY; Lewis, MS; Rosenstock, J, 2011)
"Pioglitazone was better than glibenclamide in decreasing HbA (1c), FPG, FPI, lipid profile, and in improving inflammatory parameters such as Hs-CRP, and ADN."	2.76	Pioglitazone compared to glibenclamide on lipid profile and inflammation markers in type 2 diabetic patients during an oral fat load. ( Bianchi, L; Cicero, AF; D'Angelo, A; Derosa, G; Fogari, E; Maffioli, P, 2011)
"Few studies have given suggestions on appropriate initiation insulin dosage when combined with oral antidiabetic drugs (OADs)."	2.75	Appropriate insulin initiation dosage for insulin-naive type 2 diabetes outpatients receiving insulin monotherapy or in combination with metformin and/or pioglitazone. ( Dong, JJ; Liao, L; Mou, YR; Qiu, LL; Yang, M; Zhao, JJ, 2010)
"Pioglitazone treatment reduced mean plasma fasting glucose and mean peak postprandial glucose levels."	2.73	Pioglitazone decreases fasting and postprandial endogenous glucose production in proportion to decrease in hepatic triglyceride content. ( Cobelli, C; Dalla Man, C; English, PT; Firbank, MJ; Gerrard, J; Lane, A; Ravikumar, B; Taylor, R, 2008)
"The purpose of this study was to assess the efficacy and tolerability of the dipeptidyl peptidase-4 inhibitor vildagliptin in combination with the thiazolidinedione (TZD) pioglitazone in patients with type 2 diabetes (T2DM)."	2.73	Vildagliptin in combination with pioglitazone improves glycaemic control in patients with type 2 diabetes failing thiazolidinedione monotherapy: a randomized, placebo-controlled study. ( Baron, MA; Dejager, S; Garber, AJ; Rochotte, E; Schweizer, A, 2007)
"Isohumulone treatment did not result in significant body weight gain, although pioglitazone treatment did increase body weight (10."	2.71	Isohumulones, bitter acids derived from hops, activate both peroxisome proliferator-activated receptor alpha and gamma and reduce insulin resistance. ( Ezaki, O; Fujiwara, D; Ikeshima, E; Kanaya, T; Kondo, K; Odai, H; Oikawa, S; Shiraki, M; Tsuboyama-Kasaoka, N; Yajima, H, 2004)
"Pioglitazone treatment resulted in a decrease in hemoglobin A(1c) level by 0."	2.71	Effect of pioglitazone on body composition and energy expenditure: a randomized controlled trial. ( Bray, GA; De Jonge, L; Li, Y; Smith, SR; Volaufova, J; Xie, H, 2005)
"Nonalcoholic fatty liver disease (NAFLD), the most prevalent cause of chronic liver disease worldwide, is strongly associated with obesity and insulin resistance."	2.61	Nonalcoholic Fatty Liver Disease and Obesity Treatment. ( Brunner, KT; Henneberg, CJ; Long, MT; Wilechansky, RM, 2019)
"Though gout is more prevalent in men than women, it remains unclear whether gender influences risk factors for incident gout."	2.61	Gender-specific risk factors for gout: a systematic review of cohort studies. ( Belcher, J; Evans, PL; Hay, CA; Mallen, CD; Prior, JA; Roddy, E, 2019)
"Type 2 diabetes is treated in a stepwise manner, progressing from diet and physical activity to oral antidiabetic agents and insulin."	2.45	Adding pioglitazone to insulin containing regimens in type 2 diabetes: systematic review and meta-analysis. ( Clar, C; Royle, P; Waugh, N, 2009)
"In patients with type 2 diabetes mellitus, all therapeutic options should be evaluated for their effect on cardiovascular risk factors, in addition to glycemic control."	2.42	A meta-analysis comparing the effect of thiazolidinediones on cardiovascular risk factors. ( Chiquette, E; Defronzo, R; Ramirez, G, 2004)
"Chemobrain affects up to 75% of cancer survivors, and there are no known therapeutic options for its treatment."	1.91	The Ameliorative Effect of Pioglitazone against Neuroinflammation Caused by Doxorubicin in Rats. ( Aldubayan, MA; Alhowail, AH; Almami, IS; Alsaud, MM, 2023)
" This study aimed to investigate the anti-cancer potential of PPAR-γ agonist Pioglitazone combined with COX-2 inhibitor Celelcoxib in NSCLC."	1.72	Preliminary evaluation of anticancer efficacy of pioglitazone combined with celecoxib for the treatment of non-small cell lung cancer. ( Kiran, AVVVR; Krishnamurthy, PT; Kumari, GK, 2022)
"However, insulin resistance was ameliorated by pioglitazone with or without fish oil treatment and the discontinuation of fish oil."	1.56	Impact of discontinuation of fish oil after pioglitazone-fish oil combination therapy in diabetic KK mice. ( Chiba, K; Hirako, S; Iizuka, Y; Kim, H; Matsumoto, A; Wada, M, 2020)
"Pioglitazone treatment did not influence body weight or ovarian weight in either group."	1.48	Pioglitazone is effective for multiple phenotyepes of the Zucker fa/fa rat with polycystc ovary morphology and insulin resistance. ( Baba, T; Endo, T; Honnma, H; Ikeda, K; Kiya, T; Kuno, Y; Morishita, M; Saito, T, 2018)
"Pioglitazone is an effective drug for the treatment of type 2 diabetes."	1.46	Hybrid drug combination: Anti-diabetic treatment of type 2 diabetic Wistar rats with combination of ellagic acid and pioglitazone. ( Doble, M; Nankar, RP, 2017)
"Atorvastatin treatment (Group D) abolished PPHTg which became comparable to controls, pioglitazone treatment partially blunted PPHTg resulting in intermediate PPHTg."	1.43	Postprandial Hypertriglyceridemia Predicts Development of Insulin Resistance Glucose Intolerance and Type 2 Diabetes. ( Aggarwal, S; Aslam, M; Galav, V; Madhu, SV; Sharma, KK, 2016)
"Pioglitazone was administered intragastrically once per day for 3 weeks at different doses."	1.43	The antidepressant-like effects of pioglitazone in a chronic mild stress mouse model are associated with PPARγ-mediated alteration of microglial activation phenotypes. ( Fan, Y; Peng, C; Wu, X; Xie, X; Yan, S; You, Z; Zhang, J; Zhao, Q, 2016)
"In LNCaP, a human androgen-dependent prostate cancer cell line, PGZ also inhibited cyclin D1 expression and the activation of both p38 MAPK and NFκB."	1.43	Pioglitazone, a Peroxisome Proliferator-Activated Receptor γ Agonist, Suppresses Rat Prostate Carcinogenesis. ( Kato, H; Kobayashi, M; Kuno, T; Mori, Y; Nagano, A; Nagayasu, Y; Naiki-Ito, A; Suzuki, S; Takahashi, S, 2016)
"Sporadic Alzheimer's disease (AD) is a multifactorial metabolic brain disorder characterized by progressive neurodegeneration."	1.42	Insulin sensitizers improve learning and attenuate tau hyperphosphorylation and neuroinflammation in 3xTg-AD mice. ( Blanchard, J; Gong, CX; Iqbal, K; Li, X; Li, Y; Liu, F; Yu, Y, 2015)
"Treatment with pioglitazone or nicorandil either alone or in combination successfully ameliorated the deleterious effects of HFD on the all previous parameters."	1.42	Ameliorative effect of nicorandil on high fat diet induced non-alcoholic fatty liver disease in rats. ( Elshazly, SM, 2015)
"Pioglitazone (PIO) is a peroxisome proliferator-activated receptor-γ (PPARγ) agonist in clinical use for treatment of type 2 diabetes (T2DM)."	1.42	Effects of low doses of pioglitazone on resting-state functional connectivity in conscious rat brain. ( Asin, K; Crenshaw, DG; Gottschalk, WK; Liang, Z; Roses, AD; Zhang, N, 2015)
"Rats treated with boswellic acids (125 or 250 mg/kg) or pioglitazone showed improved insulin sensitivity and a reduction in liver index, activities of liver enzymes, serum TNF-α and IL-6 as well as hepatic iNOS expression and HNE formation compared to HFD group."	1.42	Protective effect of boswellic acids versus pioglitazone in a rat model of diet-induced non-alcoholic fatty liver disease: influence on insulin resistance and energy expenditure. ( Abdelaziz, EZ; Barakat, BM; Bilasy, SE; Farag, NE; Fawzy, MS; Zaitone, SA, 2015)
"Cachexia is a multifactorial syndrome characterized by profound involuntary weight loss, fat depletion, skeletal muscle wasting, and asthenia; all symptoms are not entirely attributable to inadequate nutritional intake."	1.42	Pioglitazone treatment increases survival and prevents body weight loss in tumor-bearing animals: possible anti-cachectic effect. ( Andreotti, S; Batista, ML; Beluzi, M; Farmer, SR; Franco, FO; Henriques, FS; Knobl, P; Lima, FB; Neves, RX; Peres, SB; Santos, KB; Seelaender, M; Sertié, RA; Shida, CS, 2015)
"Pioglitazone treatment also resulted in increased expression of markers of mitochondrial biogenesis in brown adipose tissue and white adipose tissue, with mild elevations observed in animals treated with alogliptin alone."	1.40	Administration of pioglitazone alone or with alogliptin delays diabetes onset in UCD-T2DM rats. ( Bettaieb, A; Cummings, BP; Graham, JL; Haj, FG; Havel, PJ; Stanhope, K, 2014)
"Treatment with fenofibrate exerted a better effect on clinical scoring."	1.40	Fenofibrate vs pioglitazone: Comparative study of the anti-arthritic potencies of PPAR-alpha and PPAR-gamma agonists in rat adjuvant-induced arthritis. ( Jouzeau, JY; Koufany, M; Moulin, D, 2014)
"Pioglitazone ameliorates memory deficits in STZ-induced diabetic mice by reducing brain Aβ level via activation of PPARγ, which is independent of its effects on blood glucose and insulin levels."	1.39	Pioglitazone ameliorates memory deficits in streptozotocin-induced diabetic mice by reducing brain β-amyloid through PPARγ activation. ( Hong, H; Hu, M; Hu, W; Jiang, LY; Li, YQ; Liu, LP; Long, Y; Wang, C; Wang, JQ; Yan, TH; Zhang, Q, 2013)
"Pioglitazone has been shown to significantly reduce cardiovascular adverse outcomes, while preliminary data on IBTs are very encouraging as well."	1.39	Non-glycemic effects of pioglitazone and incretin-based therapies. ( Avogaro, A; Montalto, G; Rizvi, AA; Rizzo, M, 2013)
" Oral dyskinesia was induced by chronic administration of haloperidol (1 mg/kg i."	1.39	Possible beneficial effect of peroxisome proliferator-activated receptor (PPAR)--α and γ agonist against a rat model of oral dyskinesia. ( Budhiraja, RD; Grover, S; Kumar, P; Singh, K; Vikram, V, 2013)
"Adjuvant arthritis was induced by single intra-dermal injection of 0."	1.39	Anti-arthritic and anti-inflammatory activity of combined pioglitazone and prednisolone on adjuvant-induced arthritis. ( Banerjee, BD; Mediratta, PK; Negi, H; Sharma, KK; Suke, SG, 2013)
"Pioglitazone has been demonstrated to have beneficial effects on cardiovascular outcomes."	1.38	Pioglitazone attenuates cardiac fibrosis and hypertrophy in a rat model of diabetic nephropathy. ( Asker, ME; Elrashidy, RA; Mohamed, HE, 2012)
"Rosiglitazone ameliorates diabetic nephropathy by reducing the expression of chemerin and ChemR23 in diabetic rats."	1.38	Rosiglitazone ameliorates diabetic nephropathy by reducing the expression of Chemerin and ChemR23 in the kidney of streptozotocin-induced diabetic rats. ( Hu, W; Liu, D; Yu, Q; Zhang, J, 2012)
"5h and bioavailability of 85%."	1.38	NS-1: a novel partial peroxisome proliferator-activated receptor γ agonist to improve insulin sensitivity and metabolic profile. ( Chaudhary, S; Dube, A; Kothari, V; Sachan, N; Upasani, CD, 2012)
"Pioglitazone was also investigated for its effects on parameters of oxidative stress by measuring malondialdehyde (MDA) and reduced glutathione (GSH) levels in the brain."	1.38	Improvement in long term and visuo-spatial memory following chronic pioglitazone in mouse model of Alzheimer's disease. ( Gupta, LK; Gupta, R, 2012)
"Emodin is an active herbal component traditionally used in China for treating a variety of diseases."	1.38	Emodin protects against high-fat diet-induced obesity via regulation of AMP-activated protein kinase pathways in white adipose tissue. ( Chang, CJ; Liou, SS; Liu, IM; Lu, HJ; Tzeng, TF, 2012)
"Treatment of pioglitazone lowered blood glucose level and prevented delay of MNCV in SDT fatty rats."	1.38	Diabetic peripheral neuropathy in Spontaneously Diabetic Torii-Lepr(fa) (SDT fatty) rats. ( Kemmochi, Y; Matsushita, M; Mera, Y; Ohta, T; Sasase, T; Sato, E; Tadaki, H; Tomimoto, D; Yamaguchi, T, 2012)
"Insulin resistance was induced in rats by feeding a high fructose diet for 6 weeks."	1.37	Angelica acutiloba root attenuates insulin resistance induced by high-fructose diet in rats. ( Chang, CJ; Liou, SS; Liu, IM; Tzeng, TF, 2011)
"Telmisartan is an angiotensin II receptor blocker with peroxisome proliferator-activated receptor-gamma agonistic properties."	1.36	Neuroendocrine characterization and anorexigenic effects of telmisartan in diet- and glitazone-induced weight gain. ( Aubert, G; Burnier, M; Dulloo, A; Mazzolai, L; Perregaux, C; Pralong, F; Zanchi, A, 2010)
"Metformin treatment also improved hyperleptinemia, whereas pioglitazone was ineffective."	1.36	Metformin reduces body weight gain and improves glucose intolerance in high-fat diet-fed C57BL/6J mice. ( Hirasawa, Y; Ito, M; Kyuki, K; Matsui, Y; Sugiura, T; Toyoshi, T, 2010)
"Combined PIO and BEZA therapy in Type 2 diabetes does not decrease intrahepatic triglyceride content or postprandial endogenous glucose production."	1.36	Combination peroxisome proliferator-activated receptor gamma and alpha agonist treatment in Type 2 diabetes prevents the beneficial pioglitazone effect on liver fat content. ( Balasubramanian, R; Cobelli, C; Dalla Man, C; English, PT; Firbank, MJ; Gerrard, J; Lane, A; Taylor, R, 2010)
"pioglitazone treatment increased fat mass and the surface area of adipocytes more than rosiglitazone at dosages with equivalent effects on plasma glucose."	1.36	Differential modulatory effects of rosiglitazone and pioglitazone on white adipose tissue in db/db mice. ( Gang, GT; Hwang, JH; Kim, YH; Lee, CH; Noh, JR; Yang, KJ; Yang, SJ; Yeom, YI, 2010)
" These results provide a strong argument for using alogliptin in combination with pioglitazone."	1.35	The dipeptidyl peptidase-4 inhibitor alogliptin in combination with pioglitazone improves glycemic control, lipid profiles, and increases pancreatic insulin content in ob/ob mice. ( Asakawa, T; Kataoka, O; Moritoh, Y; Odaka, H; Takeuchi, K, 2009)
"Pioglitazone treatment led to reduction of the bone formation marker osteocalcin, whereas balaglitazone treatment did not affect it."	1.35	A comparison of glycemic control, water retention, and musculoskeletal effects of balaglitazone and pioglitazone in diet-induced obese rats. ( Beck-Nielsen, H; Byrjalsen, I; Christiansen, C; Henriksen, K; Karsdal, MA; Larsen, LK; Madsen, AN; Nielsen, RH, 2009)
"Pioglitazone treatment of KK-A(y) mice for 14 days significantly reduced the accumulation of inflammatory cells in ischemic myocardium, and infarct size 3 days after reperfusion compared to vehicle treatment (p<0."	1.35	Pioglitazone, a peroxisome proliferator-activated receptor-gamma agonist, attenuates myocardial ischemia-reperfusion injury in mice with metabolic disorders. ( Fuchigami, S; Hayasaki, T; Honda, T; Kaikita, K; Matsukawa, M; Ogawa, H; Sakashita, N; Sugiyama, S; Takeya, M; Tsujita, K, 2008)
"We analyzed 50 patients with type II diabetes mellitus undergoing either placebo or pioglitazone (PIO, 45 mg/day) for 16 weeks."	1.34	Reduction in hematocrit and hemoglobin following pioglitazone treatment is not hemodilutional in Type II diabetes mellitus. ( Berria, R; Cersosimo, E; Cusi, K; De Filippis, E; Defronzo, RA; Gastaldelli, A; Glass, L; Mahankali, A; Miyazaki, Y; Monroy, A, 2007)
"Pioglitazone treatment restored MCD activity to non-diabetic level and improved the restrained fatty acid metabolism in myocardial and skeletal muscles caused by insulin-resistant diabetic status."	1.33	Tissue-specific regulation of malonyl-CoA decarboxylase activity in OLETF rats. ( Ahn, CW; Cha, BS; Kim, HJ; Kim, SK; Lee, HC; Lee, YJ; Park, CW; Shim, WS; Zhao, ZS, 2006)
"Pioglitazone, or vehicle, was administered for 4 wk to 8-wk-old obese Zucker rats."	1.33	The PPARgamma agonist pioglitazone modifies the vascular sodium-angiotensin II relationship in insulin-resistant rats. ( Burnier, M; Cefai, D; Maillard, M; Nussberger, J; Perregaux, C; Zanchi, A, 2006)
"Pioglitazone is an agonist of PPARgamma, capable of reducing chronic inflammation."	1.33	Pioglitazone limits cyclosporine nephrotoxicity in rats. ( Câmara, NO; Campaholle, G; Cenedeze, MA; de Paula Antunes Teixeira, V; dos Reis, MA; Pacheco-Silva, A; Pereira, MG, 2006)
"Pioglitazone treatment during 4 weeks decreased the catalase activity in relation to the control diabetic animals."	1.32	Effect of the new thiazolidinedione-pioglitazone on the development of oxidative stress in liver and kidney of diabetic rabbits. ( Gumieniczek, A, 2003)
"Pioglitazone-treated animals showed a significant increase in GIR, reaching a similar level as the control group."	1.32	The effect of nitric oxide synthase inhibitor on improved insulin action by pioglitazone in high-fructose-fed rats. ( Han, YQ; Koshinaka, K; Ohsawa, I; Oshida, Y; Sato, Y, 2004)
"Non-alcoholic steatohepatitis (NASH) may progress to liver cirrhosis, and NASH patients with liver cirrhosis have a risk of development of hepatocellular carcinoma."	1.32	Pioglitazone prevents hepatic steatosis, fibrosis, and enzyme-altered lesions in rat liver cirrhosis induced by a choline-deficient L-amino acid-defined diet. ( Kawaguchi, K; Okita, K; Omori, K; Sakaida, I; Takami, T; Tsuchiya, M, 2004)
"Seventy-three female non-obese diabetic (NOD)/Lt mice aged 4 weeks were randomly divided into 3 groups, control group (n = 25, fed with regular diet), low dosage pioglitazone group (n = 23, pioglitazone of the concentration of 0."	1.32	[Preventive effects of pioglitazone on diabetes and relevant mechanisms, experimental study on non-obese diabetic mice]. ( He, L; Jiang, TJ; Li, X; Luo, JH; Pei, JH; Zhou, ZG, 2004)
"Treatment with pioglitazone (10 and 30 mg/kg p."	1.32	Reversal of glucose intolerance by by pioglitazone in high fat diet-fed rats. ( Kaul, CL; Patole, PS; Ramarao, P; Srinivasan, K, 2004)
"Pioglitazone (0."	1.31	Improvement of aortic wall distensibility and reduction of oxidative stress by pioglitazone in pre-diabetic stage of Otsuka Long-Evans Tokushima fatty rats. ( Kohno, M; Miyatake, A; Mizushige, K; Murakami, K; Noma, T; Tsuji, T, 2002)
"Pioglitazone was associated with statistically significant (p < 0."	1.31	Lipid response to pioglitazone in diabetic patients: clinical observations from a retrospective chart review. ( Armstrong, DU; King, AB, 2002)
"Glyburide did not increase basal or insulin-stimulated DNA synthesis."	1.30	Pioglitazone: in vitro effects on rat hepatoma cells and in vivo liver hypertrophy in KKAy mice. ( Diani, A; Messina, JL; Murray, FT; Sangani, GA; Wachowski, MB; Weinstock, RS, 1997)
"Insulin sensitivity was increased by pioglitazone hydrochloride (P = 0."	1.29	Pioglitazone increases insulin sensitivity, reduces blood glucose, insulin, and lipid levels, and lowers blood pressure, in obese, insulin-resistant rhesus monkeys. ( Baum, ST; Bergman, RN; Elson, DF; Kemnitz, JW; Meglasson, MD; Roecker, EB, 1994)
"The effects of dietary fructose alone or in combination with a new oral agent, pioglitazone, on VLDL-triglyceride (TG) turnover were studied in genetically obese Wistar fatty rats characterized by hyperinsulinemia (7,488 +/- 954 pmol/l), hyperglycemia, (22."	1.29	VLDL triglyceride kinetics in Wistar fatty rats, an animal model of NIDDM: effects of dietary fructose alone or in combination with pioglitazone. ( Amano, N; Ebara, T; Hirano, T; Hozumi, T; Ishida, Y; Kazumi, T; Odaka, H; Yoshino, G, 1996)

Research

Studies (214)

Authors

Clinical Trials (34)

Trial Overview

Trial Outcomes

Change From Baseline (BL) in Glycosylated Hemoglobin (HbA1c) at Week 52

Timeframe	Studies, this research(%)	All Research%
pre-1990	0 (0.00)	18.7374
1990's	10 (4.67)	18.2507
2000's	81 (37.85)	29.6817
2010's	114 (53.27)	24.3611
2020's	9 (4.21)	2.80

Authors	Studies
Zhang, JQ	1
Li, SM	1
Ma, X	1
Zhong, G	1
Chen, R	1
Li, XS	1
Zhu, GF	1
Zhou, B	1
Guo, B	1
Wu, HS	1
Tang, L	1
Katahira, S	1
Sugimura, Y	1
Grupp, S	1
Doepp, R	1
Selig, JI	1
Barth, M	1
Lichtenberg, A	1
Akhyari, P	1
Abdalla, MA	1
Shah, N	1
Deshmukh, H	1
Sahebkar, A	1
Östlundh, L	1
Al-Rifai, RH	1
Atkin, SL	2
Sathyapalan, T	1
Alsaud, MM	1
Alhowail, AH	1
Aldubayan, MA	1
Almami, IS	1
Pei, Y	1
Liu, YY	1
Sun, M	1
Zheng, J	1
Zhou, TT	1
Wang, B	1
Hu, H	1
Wang, ZL	1
Higuchi, T	1
Sugisawa, N	1
Miyake, K	1
Oshiro, H	1
Yamamoto, N	1
Hayashi, K	1
Kimura, H	1
Miwa, S	1
Igarashi, K	1
Kline, Z	1
Bouvet, M	1
Singh, SR	1
Tsuchiya, H	2
Hoffman, RM	1
Iizuka, Y	1
Chiba, K	1
Kim, H	1
Hirako, S	1
Wada, M	1
Matsumoto, A	1
Blazina, I	1
Selph, S	1
Hegazy, M	1
El-Shafey, M	1
Abulsoud, AI	1
Elsadek, BEM	1
Abd Elaziz, AI	1
Salama, SA	1
Lian, J	1
Fu, J	2
Kumari, GK	2
Kiran, AVVVR	2
Krishnamurthy, PT	2
Abdul-Ghani, M	2
Migahid, O	1
Megahed, A	1
DeFronzo, RA	5
Zirie, M	1
Jayyousi, A	1
Simeone, TA	1
Matthews, SA	1
Simeone, KA	1
Home, PD	1
Ahrén, B	2
Reusch, JEB	1
Rendell, M	1
Weissman, PN	1
Cirkel, DT	1
Miller, D	1
Ambery, P	1
Carr, MC	1
Nauck, MA	1
Ito, D	1
Shimizu, S	1
Inoue, K	1
Saito, D	1
Yanagisawa, M	1
Inukai, K	1
Akiyama, Y	1
Morimoto, Y	2
Noda, M	1
Shimada, A	1
Suzuki, D	1
Saito-Hakoda, A	1
Ito, R	1
Shimizu, K	1
Parvin, R	1
Shimada, H	1
Noro, E	1
Suzuki, S	4
Fujiwara, I	1
Kagechika, H	1
Rainey, WE	1
Kure, S	1
Ito, S	1
Yokoyama, A	1
Sugawara, A	1
Nankar, RP	1
Doble, M	1
Hussain, M	1
Shad, MN	1
Akhtar, L	1
Li, J	2
Xu, B	1
Chen, Z	1
Zhou, C	1
Liao, L	2
Qin, Y	2
Yang, C	1
Zhang, X	2
Hu, Z	1
Sun, L	1
Zhu, D	2
Xie, P	1
Morishita, M	2
Endo, T	1
Baba, T	1
Kuno, Y	1
Ikeda, K	1
Kiya, T	1
Honnma, H	1
Saito, T	3
Patel, R	1
Shah, G	1
Cho, KY	1
Nakamura, A	2
Omori, K	2
Takase, T	1
Miya, A	1
Manda, N	1
Kurihara, Y	1
Aoki, S	1
Atsumi, T	1
Miyoshi, H	1
Shawky, NM	1
Shehatou, GSG	1
Suddek, GM	1
Gameil, NM	1
Brunner, KT	1
Henneberg, CJ	1
Wilechansky, RM	1
Long, MT	1
Evans, PL	1
Prior, JA	1
Belcher, J	1
Hay, CA	1
Mallen, CD	1
Roddy, E	1
Maffioli, P	5
Fogari, E	2
D'Angelo, A	4
Perrone, T	1
Derosa, G	5
Liu, LP	1
Yan, TH	1
Jiang, LY	1
Hu, W	2
Hu, M	2
Wang, C	1
Zhang, Q	2
Long, Y	1
Wang, JQ	1
Li, YQ	1
Hong, H	1
Bray, GA	2
Smith, SR	2
Banerji, MA	1
Tripathy, D	1
Clement, SC	1
Buchanan, TA	2
Henry, RR	2
Kitabchi, AE	1
Mudaliar, S	2
Musi, N	1
Ratner, RE	1
Schwenke, DC	1
Stentz, FB	1
Reaven, PD	1
Joerin, L	1
Kauschka, M	1
Bonnländer, B	1
Pischel, I	1
Benedek, B	1
Butterweck, V	1
Rizzo, M	1
Avogaro, A	1
Montalto, G	1
Rizvi, AA	1
Yang, SC	1
Tseng, HL	1
Shieh, KR	1
Lee, JO	1
Auger, C	1
Park, DH	1
Kang, M	1
Oak, MH	1
Kim, KR	1
Schini-Kerth, VB	1
Bhansali, S	1
Shafiq, N	1
Pandhi, P	1
Singh, AP	1
Singh, I	1
Singh, PK	1
Sharma, S	1
Malhotra, S	1
Kovacs, CS	2
Seshiah, V	2
Swallow, R	1
Jones, R	1
Rattunde, H	1
Woerle, HJ	2
Broedl, UC	2
Grover, S	1
Kumar, P	2
Singh, K	1
Vikram, V	1
Budhiraja, RD	1
Zenari, L	1
Marangoni, A	1
Zhao, ZQ	1
Luo, R	1
Li, LY	1
Tian, FS	1
Zheng, XL	1
Xiong, HL	1
Sun, LT	1
Suke, SG	1
Negi, H	1
Mediratta, PK	1
Banerjee, BD	1
Sharma, KK	2
Malekinejad, H	1
Mehrabi, M	1
Khoramjouy, M	1
Rezaei-Golmisheh, A	1
Masuda, T	1
Fu, Y	1
Eguchi, A	1
Czogalla, J	1
Rose, MA	1
Kuczkowski, A	1
Gerasimova, M	1
Feldstein, AE	1
Scadeng, M	1
Vallon, V	2
Konda, VR	1
Desai, A	1
Darland, G	1
Grayson, N	1
Bland, JS	1
Cummings, BP	1
Bettaieb, A	1
Graham, JL	1
Stanhope, K	1
Haj, FG	1
Havel, PJ	1
Koufany, M	1
Jouzeau, JY	1
Moulin, D	1
Takada, S	1
Hirabayashi, K	1
Kinugawa, S	1
Yokota, T	1
Matsushima, S	1
Suga, T	1
Kadoguchi, T	1
Fukushima, A	1
Homma, T	1
Mizushima, W	1
Masaki, Y	1
Furihata, T	1
Katsuyama, R	1
Okita, K	2
Tsutsui, H	1
Niture, NT	1
Ansari, AA	1
Naik, SR	1
Yu, Y	2
Li, X	2
Blanchard, J	1
Li, Y	3
Iqbal, K	1
Liu, F	1
Gong, CX	1
Elshazly, SM	1
Watanabe, Y	1
Nakayama, K	1
Taniuchi, N	1
Horai, Y	1
Kuriyama, C	1
Ueta, K	1
Arakawa, K	1
Senbonmatsu, T	1
Shiotani, M	1
Zhu, C	1
Xiao, Y	2
Liu, X	1
Han, J	1
Zhang, J	3
Wei, L	2
Jia, W	1
Crenshaw, DG	1
Asin, K	1
Gottschalk, WK	1
Liang, Z	1
Zhang, N	1
Roses, AD	1
Ibrahim, SM	1
El-Denshary, ES	1
Abdallah, DM	1
Zaitone, SA	1
Barakat, BM	1
Bilasy, SE	1
Fawzy, MS	1
Abdelaziz, EZ	1
Farag, NE	1
Beluzi, M	1
Peres, SB	1
Henriques, FS	1
Sertié, RA	1
Franco, FO	1
Santos, KB	1
Knobl, P	1
Andreotti, S	1
Shida, CS	1
Neves, RX	1
Farmer, SR	1
Seelaender, M	1
Lima, FB	1
Batista, ML	1
Merker, L	1
Christiansen, AV	1
Roux, F	1
Salsali, A	2
Kim, G	1
Stella, P	1
Li, R	1
Xu, W	1
Luo, S	1
Xu, H	1
Tong, G	1
Zeng, L	1
Weng, J	1
Aslam, M	1
Aggarwal, S	1
Galav, V	1
Madhu, SV	1
Vu, A	1
Kosmiski, LA	1
Beitelshees, AL	1
Prigeon, R	1
Sidhom, MS	1
Bredbeck, B	1
Predhomme, J	1
Deininger, KM	1
Aquilante, CL	1
Abd El-Haleim, EA	1
Bahgat, AK	1
Saleh, S	1
Del Prato, S	1
Chilton, R	1
Jain, S	1
Sharma, B	1
Zhao, Q	1
Wu, X	1
Yan, S	1
Xie, X	1
Fan, Y	1
Peng, C	1
You, Z	1
Li, YC	1
Liu, YM	1
Shen, JD	1
Chen, JJ	1
Pei, YY	1
Fang, XY	1
Broglio, F	1
Mannucci, E	1
Napoli, R	1
Nicolucci, A	1
Purrello, F	1
Nikonova, E	1
Stager, W	1
Trevisan, R	1
Mori, Y	2
Nagano, A	1
Naiki-Ito, A	1
Kato, H	1
Nagayasu, Y	1
Kobayashi, M	1
Kuno, T	1
Takahashi, S	1
Ravikumar, B	1
Gerrard, J	2
Dalla Man, C	2
Firbank, MJ	2
Lane, A	2
English, PT	2
Cobelli, C	2
Taylor, R	2
Wu, ZH	1
Zhao, SP	1
Chu, LX	1
Ye, HJ	1
Ye, Y	3
Lin, Y	2
Perez-Polo, JR	2
Birnbaum, Y	3
Moritoh, Y	2
Takeuchi, K	2
Asakawa, T	2
Kataoka, O	2
Odaka, H	4
Sugimoto, M	1
Arai, H	1
Tamura, Y	1
Murayama, T	1
Khaengkhan, P	1
Nishio, T	1
Ono, K	1
Ariyasu, H	1
Akamizu, T	1
Ueda, Y	1
Kita, T	1
Harada, S	1
Kamei, K	1
Yokode, M	1
Ghaisas, M	1
Navghare, V	1
Takawale, A	1
Zope, V	1
Tanwar, M	1
Deshpande, A	1
Laurent, D	1
Gounarides, JS	1
Gao, J	1
Boettcher, BR	1
Akiyama, M	1
Hatanaka, M	1
Ohta, Y	1
Ueda, K	1
Yanai, A	1
Uehara, Y	1
Tanabe, K	1
Tsuru, M	1
Miyazaki, M	1
Saeki, S	1
Shinoda, K	1
Oka, Y	1
Tanizawa, Y	1
Toblli, JE	1
Ferrini, MG	1
Cao, G	1
Vernet, D	1
Angerosa, M	1
Gonzalez-Cadavid, NF	1
Mikhail, N	1
Bolli, G	2
Dotta, F	2
Colin, L	1
Minic, B	1
Goodman, M	1
Clar, C	1
Royle, P	1
Waugh, N	1
Henriksen, K	1
Byrjalsen, I	1
Nielsen, RH	1
Madsen, AN	1
Larsen, LK	1
Christiansen, C	1
Beck-Nielsen, H	1
Karsdal, MA	1
Kiyici, S	1
Ersoy, C	1
Oz Gul, O	1
Sarandol, E	1
Demirci, M	1
Tuncel, E	1
Sigirli, D	1

Trial	Phase	Enrollment	Study Type	Start Date	Status
A Randomized, Double-Blind, Placebo-Controlled, Parallel-Group, Multicenter Study to Determine the Efficacy and Safety of Albiglutide When Used in Combination With Pioglitazone With or Without Metformin in Subjects With Type 2 Diabetes Mellitus[NCT00849056]	Phase 3	310 participants (Actual)	Interventional	2009-01-31	Completed
A Randomized, Open-label, Parallel-group, Multicenter Study to Determine the Efficacy and Long-term Safety of Albiglutide Compared With Insulin in Subjects With Type 2 Diabetes Mellitus.[NCT00838916]	Phase 3	779 participants (Actual)	Interventional	2009-02-28	Completed
A Randomized, Double-Blind, Placebo-Controlled, Parallel-Group, Multicenter Study to Determine the Efficacy and Safety of Two Dose Levels of Albiglutide Compared With Placebo in Subjects With Type 2 Diabetes Mellitus[NCT00849017]	Phase 3	309 participants (Actual)	Interventional	2009-01-31	Completed
A Randomized, Double-blind, Placebo and Active-Controlled, Parallel-group, Multicenter Study to Determine the Efficacy and Safety of Albiglutide Administered in Combination With Metformin and Glimepiride Compared With Metformin Plus Glimepiride and Placeb[NCT00839527]	Phase 3	685 participants (Actual)	Interventional	2009-02-28	Completed
A Randomized, Double-Blind, Placebo and Active-Controlled, Parallel-Group, Multicenter Study to Determine the Efficacy and Safety of Albiglutide When Used in Combination With Metformin Compared With Metformin Plus Sitagliptin, Metformin Plus Glimepiride, [NCT00838903]	Phase 3	1,049 participants (Actual)	Interventional	2009-02-28	Completed
Calisthenics Versus High-intensity Interval Exercises on Health-related Outcomes in Patients With Non-alcoholic Fatty Liver[NCT06032650]		60 participants (Anticipated)	Interventional	2023-10-31	Not yet recruiting
Multicenter, Randomized, Double Blind, Placebo-controlled, Phase II Clinical Trial to Evaluate the Safety and Efficacy of YJP-14 Capsules for the Treatment of Endothelial Dysfunction in Patients With Diabetes Mellitus[NCT01836172]	Phase 2	136 participants (Anticipated)	Interventional	2013-04-30	Active, not recruiting
Effect of Gymnema Sylvestre Administration on Metabolic Syndrome, Insulin Sensitivity and Insulin Secretion[NCT02370121]	Phase 2	24 participants (Actual)	Interventional	2013-02-28	Completed
SGLT-2 Inhibitor Empagliflozin Effects on Appetite and Weight Regulation: A Randomised Double-blind Placebo-controlled Trial (The SEESAW Study)[NCT02798744]	Phase 4	68 participants (Actual)	Interventional	2016-12-31	Completed
A Prospective, Randomized, Parallel-group, Adaptive Design Phase IIb/III, Multicenter Study, to Assess the Efficacy of Polychemotherapy for Inducing Remission of Newly Diagnosed Type 2 Diabetes.[NCT04271189]	Phase 2/Phase 3	180 participants (Anticipated)	Interventional	2020-09-01	Active, not recruiting
A Randomised, Double-blind, Placebo-controlled Parallel Group Efficacy and Safety Trial of BI 10773 (10 and 25 mg Administered Orally Once Daily) Over 24 Weeks in Patients With Type 2 Diabetes Mellitus With Insufficient Glycaemic Control Despite a Backgro[NCT01210001]	Phase 3	499 participants (Actual)	Interventional	2010-09-30	Completed
Effect of the Antidiabetic Drug DAPAgliflozin on the Coronary Macrovascular and MICROvascular Function in Type 2 Diabetic Patients[NCT05392959]	Phase 4	100 participants (Anticipated)	Interventional	2022-06-06	Recruiting
Dipeptidyl Peptidase-4 Inhibition and Narrow-band Ultraviolet-B Light in Psoriasis (DINUP): A Randomised Clinical Trial[NCT02347501]	Phase 2	118 participants (Actual)	Interventional	2013-11-30	Completed
Dipeptidyl Peptidase-4 Inhibition in Psoriasis Patients With Diabetes (DIP): A Randomized Clinical Trial.[NCT01991197]	Phase 2	20 participants (Actual)	Interventional	2014-04-30	Completed
Effects of the PPAR-gamma Agonist Pioglitazone on Renal and Hormonal Responses to Salt in Diabetic and Hypertensive Subjects[NCT01090752]	Phase 4	16 participants (Actual)	Interventional	2005-10-31	Completed
The Effect of Adding Vildagliptin Versus Glimepiride to Metformin on Markers of Inflammation, Thrombosis, and Atherosclerosis in Diabetic Patients With Symptomatic Coronary Artery Diseases[NCT03693560]	Phase 4	80 participants (Actual)	Interventional	2018-10-08	Completed
Effects of Vildagliptin/Metformin Combination on Markers of Atherosclerosis, Thrombosis, and Inflammation in Diabetic Patients With Coronary Artery Disease[NCT01604213]	Phase 4	60 participants (Actual)	Interventional	2012-09-30	Completed
A Randomized Trial Comparing Exenatide With Placebo in Subjects With Type 2 Diabetes on Insulin Glargine With or Without Oral Antihyperglycemic Medications[NCT00765817]	Phase 3	261 participants (Actual)	Interventional	2008-10-31	Completed
Exenatide BID Compared With Insulin Glargine to Change Liver Fat Content in Non-alcoholic Fatty-liver Disease Patients With Type 2 Diabetes[NCT02303730]	Phase 4	76 participants (Actual)	Interventional	2015-03-31	Completed
Effect of Exenatide Treatment on Hepatic Fat Content and Plasma Adipocytokine Levels in Patients With Type 2 Diabetes Mellitus[NCT01432405]	Phase 4	24 participants (Actual)	Interventional	2007-06-30	Completed
PROspective PioglitAzone Clinical Trial In MacroVascular Events: A Macrovascular Outcome Study in Type 2 Diabetic Patients Comparing Pioglitazone With Placebo in Addition to Existing Therapy[NCT00174993]	Phase 3	4,373 participants (Actual)	Interventional	2001-05-31	Completed
Effect of Anti-diabetic Drugs on Glycemic Variability. A Comparison Between Gliclazide MR (Modified Release) and Dapagliflozin on Glycemic Variability Measured by Continuous Glucose Monitoring (CGM) in Patients With Uncontrolled Type 2 Diabetes[NCT02925559]	Phase 4	135 participants (Actual)	Interventional	2016-10-31	Completed
Effect of Dapagliflozin Administration on Metabolic Syndrome, Insulin Sensitivity, and Insulin Secretion[NCT02113241]	Phase 2/Phase 3	24 participants (Actual)	Interventional	2014-04-30	Completed
A Multicenter, Randomized, Double-Blind, Placebo-Controlled, Parallel Group, Phase 3 Trial to Evaluate the Safety and Efficacy of Dapagliflozin in Combination With Thiazolidinedione Therapy in Subjects With Type 2 Diabetes Who Have Inadequate Glycemic Con[NCT00683878]	Phase 3	972 participants (Actual)	Interventional	2008-07-31	Completed
Effectiveness of the Treatment With Dapagliflozin and Metformin Compared to Metformin Monotherapy for Weight Loss on Diabetic and Prediabetic Patients With Obesity Class III[NCT03968224]	Phase 2/Phase 3	90 participants (Anticipated)	Interventional	2018-07-07	Recruiting
Effect of Saxagliptin in Addition to Dapagliflozin and Metformin on Insulin Resistance, Islet Cell Dysfunction, and Metabolic Control in Subjects With Type 2 Diabetes Mellitus on Previous Metformin Treatment[NCT02304081]	Phase 4	64 participants (Actual)	Interventional	2015-01-31	Completed
Modulation of Insulin Secretion and Insulin Sensitivity in Bangladeshi Type 2 Diabetic Subjects by an Insulin Sensitizer Pioglitazone and T2DM Association With PPARG Gene Polymorphism.[NCT01589445]	Phase 4	77 participants (Actual)	Interventional	2008-11-30	Completed
Effects of Pioglitazone on Reverse Cholesterol Transport and HDL Function in Persons With Diabetes[NCT01156597]	Phase 3	30 participants (Actual)	Interventional	2008-04-30	Completed
Role of Pioglitazone and Berberine in Treatment of Non-alcoholic Fatty Liver Disease(NAFLD) Patients With Impaired Glucose Regulation or Type 2 Diabetes Mellitus[NCT00633282]	Phase 2	184 participants (Actual)	Interventional	2008-03-31	Completed
A Study on the Effects of Peroxisome Proliferators Activated Receptor-γ Agonists on Certain Biochemical and Inflammatory Markers in Patients With Metabolic Syndrome[NCT00926341]	Phase 4	110 participants (Actual)	Interventional	2006-10-31	Completed
Efficacy and Safety of Vildagliptin in Combination With Pioglitazone in Patients With Type 2 Diabetes[NCT00099853]	Phase 3	362 participants (Actual)	Interventional	2004-05-31	Completed
Efficacy and Safety of Vildagliptin in Combination With Pioglitazone in Drug Naive Patients With Type 2 Diabetes[NCT00101803]	Phase 3	527 participants (Actual)	Interventional	2005-01-31	Completed
Vildagliptin Compared to Pioglitazone in Combination With Metformin in Patients With Type 2 Diabetes[NCT00237237]	Phase 3	588 participants	Interventional	2005-10-31	Completed
Effects of Sitagliptin on Postprandial Glycaemia, Incretin Hormones and Blood Pressure in Type 2 Diabetes - Relationship to Gastric Emptying[NCT02324010]	Phase 2	14 participants (Actual)	Interventional	2015-07-31	Completed
[information is prepared from clinicaltrials.gov, extracted Sep-2024]

HbA1c is a form of hemoglobin that is measured primarily to identify the average plasma glucose concentration over a 2- to 3-month period. The BL HbA1c value is defined as the last non-missing value before the start of treatment. Change from BL was calculated as the value at Week 52 minus the value at BL. Based on analysis of covariance (ANCOVA): change = treatment + BL HbA1c + prior myocardial infarction history + age category + region + current antidiabetic therapy. The last observation carried forward (LOCF) method was used to impute missing post-BL HbA1c values; the last non-missing post-BL on-treatment measurement was used to impute the missing measurement. HbA1c values obtained after hyperglycemic rescue were treated as missing and were replaced with pre-rescue values. One Intent-to-Treat (ITT) participant (par.) had all post-BL HbA1c measurements occur after hyperglycemic rescue. This par. is included in the ITT Population counts but did not contribute to this analysis. (NCT00849056)
Timeframe: Baseline and Week 52

Change From Baseline in Body Weight at Week 156

Intervention	Percentage of HbA1c in the blood (Least Squares Mean)
Placebo + Pioglitazone With or Without Metformin	-0.05
Albiglutide 30 mg + Pioglitazone With or Without Metformin	-0.81

The Baseline value is the last non-missing value before the start of treatment. Change from Baseline was calculated as the post-Baseline weight minus the Baseline weight. (NCT00849056)
Timeframe: Baseline and Week 156

Change From Baseline in Body Weight at Week 52

Intervention	Kilograms (Mean)
Placebo + Pioglitazone With or Without Metformin	1.50
Albiglutide 30 mg + Pioglitazone With or Without Metformin	-0.16

The Baseline value is the last non-missing value before the start of treatment. Change from Baseline was calculated as the post-Baseline weight minus the Baseline weight. The LOCF method was used to impute missing post-Baseline weight values. Weight values obtained after hyperglycemia rescue were treated as missing and replaced with prerescue values. Based on ANCOVA: change = treatment + Baseline weight + prior myocardial infarction history + age category + region + current antidiabetic therapy. (NCT00849056)
Timeframe: Baseline and Week 52

Change From Baseline in Fasting Plasma Glucose (FPG) at Week 156

Intervention	Kilograms (Least Squares Mean)
Placebo + Pioglitazone With or Without Metformin	0.45
Albiglutide 30 mg + Pioglitazone With or Without Metformin	0.28

The Baseline FPG value is the last non-missing value before the start of treatment. Change from Baseline was calculated as the post-Baseline FPG minus the Baseline FPG. (NCT00849056)
Timeframe: Baseline and Week 156

Change From Baseline in Fasting Plasma Glucose (FPG) at Week 52

Intervention	Millimoles per liter (mmol/L) (Mean)
Placebo + Pioglitazone With or Without Metformin	0.03
Albiglutide 30 mg + Pioglitazone With or Without Metformin	-1.26

The FPG test measures blood sugar levels after the participant has not eaten (fasted) for 12 to 14 hours. The Baseline FPG value is the last non-missing value before the start of treatment. The LOCF method was used to impute missing post-Baseline FPG values. FPG values obtained after hyperglycemia rescue were treated as missing and replaced with pre-rescue values. Change from Baseline was calculated as the post-Baseline value minus the Baseline value. Based on ANCOVA: change = treatment + Baseline weight + prior myocardial infarction history + age category + region + current antidiabetic therapy. (NCT00849056)
Timeframe: Baseline and Week 52

Time to Hyperglycemia Rescue

Intervention	Millimoles per liter (mmol/L) (Least Squares Mean)
Placebo + Pioglitazone With or Without Metformin	0.35
Albiglutide 30 mg + Pioglitazone With or Without Metformin	-1.28

Participants who experienced persistent hyperglycemia (high blood glucose) could have qualified for hyperglycemia rescue. The conditions for hyperglycemia rescue were as follows: FPG >=280 milligrams/deciliter (mg/dL) between >=Week 2 and =250 mg/dL between >=Week 4 and =8.5% and a <=0.5% reduction from Baseline between >=Week 12 and =8.5% between >=Week 24 and =8.0% between >= Week 48 and NCT00849056)
Timeframe: From the start of study medication until the end of the treatment (up to Week 156)

Change From Baseline in HbA1c at Weeks 104 and 156

Intervention	Weeks (Median)
Placebo + Pioglitazone With or Without Metformin	52.86
Albiglutide 30 mg + Pioglitazone With or Without Metformin	NA

HbA1c is a form of hemoglobin that is measured primarily to identify the average plasma glucose concentration over a 2- to 3-month period. Baseline HbA1c value is defined as the last non-missing value before the start of treatment. Change from Baseline was calculated as the post-Baseline value minus the Baseline value. This analysis used observed HbA1c values, excluding those obtained after hyperglycemia rescue; no missing data imputation was performed. (NCT00849056)
Timeframe: Baseline and Weeks 104 and 156

Number of Participants Who Achieved Clinically Meaningful HbA1c Response Levels of <6.5%, <7%, and <7.5% at Week 156

Intervention	Percentage of HbA1c in the blood (Mean)
	Week 104, n= 29, 72	Week 156, n=26, 54
Albiglutide 30 mg + Pioglitazone With or Without Metformin	-0.92	-0.87
Placebo + Pioglitazone With or Without Metformin	-0.72	-0.50

The number of participants who achieved the HbA1c treatment goal (i.e., HbA1c response levels of <6.5%, <6.5%, and <7.0% at Week 156) were assessed. (NCT00849056)
Timeframe: Week 156

Number of Participants Who Achieved Clinically Meaningful HbA1c Response Levels of <6.5%, <7%, and <7.5% at Week 52

Intervention	Participants (Number)
	HbA1c <6.5%	HbA1c <7%	HbA1c <7.5%
Albiglutide 30 mg + Pioglitazone With or Without Metformin	20	32	44
Placebo + Pioglitazone With or Without Metformin	7	12	17

The number of participants who achieved the HbA1c treatment goal (i.e., HbA1c response levels of <6.5%, <6.5%, and <7.0% at Week 52) were assessed. (NCT00849056)
Timeframe: Week 52

Change From Baseline (BL) in Glycosylated Hemoglobin (HbA1c) at Week 52

Intervention	Participants (Number)
	HbA1c <6.5%	HbA1c <7%	HbA1c <7.5%
Albiglutide 30 mg + Pioglitazone With or Without Metformin	37	66	96
Placebo + Pioglitazone With or Without Metformin	8	22	44

HbA1c is a form of hemoglobin that is measured primarily to identify the average plasma glucose concentration over a 2- to 3-month period. The BL HbA1c value is defined as the last non-missing value before the start of treatment. Change from BL was calculated as the value at Week 52 minus the value at BL. Based on analysis of covariance (ANCOVA): change = treatment + BL HbA1c + prior myocardial infarction history + age category + region + current antidiabetic therapy. Difference of least squares means (albiglutide - insulin glargine) is from the ANCOVA model. The last observation carried forward (LOCF) method was used to impute missing post-Baseline HbA1c values; the last non-missing post-BL on-treatment measurement was used to impute the missing measurement. HbA1c values obtained after hyperglycemic rescue were treated as missing and were replaced with pre-rescue values. (NCT00838916)
Timeframe: Baseline and Week 52

Change From Baseline in Body Weight at Week 156

Intervention	Percentage of HbA1c in the blood (Least Squares Mean)
Albiglutide 30 mg + Metformin +/- Sulfonylurea	-0.67
Insulin Glargine 10 Units + Metformin +/- Sulfonylurea	-0.79

Change From Baseline in Body Weight at Week 52

Intervention	Kilograms (Mean)
Albiglutide 30 mg + Metformin +/- Sulfonylurea	-3.47
Insulin Glargine 10 Units + Metformin +/- Sulfonylurea	0.90

The Baseline value is the last non-missing value before the start of treatment. Change from Baseline was calculated as the post-Baseline weight minus the Baseline weight. The LOCF method was used to impute missing post-Baseline weight values. Weight values obtained after hyperglycemia rescue were treated as missing and replaced with prerescue values. Based on ANCOVA: change = treatment + Baseline weight + Baseline HbA1c category + prior myocardial infarction history + age category + region + current antidiabetic therapy. (NCT00838916)
Timeframe: Baseline and Week 52

Change From Baseline in Fasting Plasma Glucose (FPG) at Week 156

Intervention	Kilograms (Least Squares Mean)
Albiglutide 30 mg + Metformin +/- Sulfonylurea	-1.05
Insulin Glargine 10 Units + Metformin +/- Sulfonylurea	1.56

The FPG test measures blood sugar levels after the participant has not eaten (fasted) for 12 to 14 hours. The Baseline FPG value is the last non-missing value before the start of treatment. Change from Baseline was calculated as the post-Baseline value minus the Baseline value. (NCT00838916)
Timeframe: Baseline and Week 156

Change From Baseline in Fasting Plasma Glucose (FPG) at Week 52

Intervention	Millimoles per liter (mmol/L) (Mean)
Albiglutide 30 mg + Metformin +/- Sulfonylurea	-0.83
Insulin Glargine 10 Units + Metformin +/- Sulfonylurea	-2.19

The FPG test measures blood sugar levels after the participant has not eaten (fasted) for 12 to 14 hours. The Baseline FPG value is the last non-missing value before the start of treatment. The LOCF method was used to impute missing post-Baseline FPG values. FPG values obtained after hyperglycemia rescue were treated as missing and replaced with pre-rescue values. Change from Baseline was calculated as the post-Baseline value minus the Baseline value. Based on ANCOVA: change = treatment + Baseline FPG + Baseline HbA1c category + prior myocardial infarction history + age category + region + current antidiabetic therapy. (NCT00838916)
Timeframe: Baseline and Week 52

Change From Baseline in Glucose Profile Measured by 24-hour Area Under Curve (AUC) at Week 52

Intervention	Millimoles per liter (mmol/L) (Least Squares Mean)
Albiglutide 30 mg + Metformin +/- Sulfonylurea	-0.87
Insulin Glargine 10 Units + Metformin +/- Sulfonylurea	-2.06

A 24-hour glucose profile was collected at Baseline and Week 52 at a subset of sites in a subset of participants per treatment group using the continuous glucose monitoring device. Glucose measurements were obtained at 5 minute increments in the 24-hour period. The area under the curve (AUC) was determined using the trapezoidal method on the measurements obtained during the first 24 hours of continuous monitoring. This analysis used observed values excluding those obtained after hyperglycemia rescue; no missing data imputation was performed. The Baseline value is the last non-missing value before the start of treatment. (NCT00838916)
Timeframe: Baseline and Week 52

Change From Baseline in HbA1c at Week 156

Intervention	Millimoles per hour per liter (mmol.h/L) (Mean)
Albiglutide 30 mg + Metformin +/- Sulfonylurea	0.457
Insulin Glargine 10 Units + Metformin +/- Sulfonylurea	-1.657

Time to Hyperglycemia Rescue

Intervention	Percentage of HbA1c in the blood (Mean)
Albiglutide 30 mg + Metformin +/- Sulfonylurea	-0.83
Insulin Glargine 10 Units + Metformin +/- Sulfonylurea	-1.00

Participants who experienced persistent hyperglycemia (high blood glucose) could have qualified for hyperglycemia rescue. The conditions for hyperglycemia rescue were as follows: FPG >=280 milligrams/deciliter (mg/dL) between >=Week 2 and =250 mg/dL between >=Week 4 and =8.5% and a <=0.5% reduction from Baseline between >=Week 12 and =8.5% between >=Week 24 and =8.0% between >= Week 48 and NCT00838916)
Timeframe: From the start of study medication until the end of the treatment (up to Week 156)

Albiglutide Plasma Concentrations at Week 8 and Week 24

Intervention	Weeks (Median)
Albiglutide 30 mg + Metformin +/- Sulfonylurea	107.57
Insulin Glargine 10 Units + Metformin +/- Sulfonylurea	NA

Albiglutide plasma concentration data was analyzed at Week 8 pre-dose, Week 8 post-dose, Week 24 pre-dose and Week 24 post-dose. All participants receiving albiglutide were initiated on a 30 mg weekly dosing regimen; however, beginning at Week 4, uptitration of albiglutide was allowed based on glycemic response. As such, albiglutide plasma concentrations achieved at each sampling time represent a mixed population of participants receiving either 30 mg or 50 mg weekly for various durations. (NCT00838916)
Timeframe: Weeks 8 and 24

Number of Participants Who Achieved Clinically Meaningful HbA1c Response Levels of <6.5%, <7%, and <7.5% at Week 156

Intervention	nanograms/milliliter (ng/mL) (Mean)
	Week 8, Pre-dose, n=408	Week 8, Post-dose, n=398	Week 24, Pre-dose, n=416	Week 24, Post-dose, n=401
Albiglutide 30 mg + Metformin +/- Sulfonylurea	1642.83	1911.35	2159.30	2748.15

The number of participants who achieved the HbA1c treatment goal (i.e., HbA1c response levels of <6.5%, <7%, and <7.5% at Week 156) were assessed. (NCT00838916)
Timeframe: Week 156

Number of Participants Who Achieved Clinically Meaningful HbA1c Response Levels of <6.5%, <7%, and <7.5% at Week 52

Intervention	Participants (Number)
	HbA1c <6.5%	HbA1c <7%	HbA1c <7.5%
Albiglutide 30 mg + Metformin +/- Sulfonylurea	33	59	85
Insulin Glargine 10 Units + Metformin +/- Sulfonylurea	18	46	71

The number of participants who achieved the HbA1c treatment goal (i.e., HbA1c response levels of <6.5%, <7%, and <7.5% at Week 52) were assessed. (NCT00838916)
Timeframe: Week 52

Change From Baseline (BL) in Glycosylated Hemoglobin (HbA1c) at Week 52

Intervention	Participants (Number)
	HbA1c <6.5%	HbA1c <7%	HbA1c <7.5%
Albiglutide 30 mg + Metformin +/- Sulfonylurea	54	156	268
Insulin Glargine 10 Units + Metformin +/- Sulfonylurea	25	78	135

Glycated hemoglobin (HbA1c) is a form of hemoglobin that is measured primarily to identify the average plasma glucose concentration over a 2- to 3-month period. The BL HbA1c is defined as the last non-missing value before the start of treatment. Change from BL was calculated as the value at Week 52 minus the value at BL. The analysis was performed using an Analysis of Covariance (ANCOVA) model with treatment group, region, history of prior myocardial infarction (yes versus no), and age category (<65 years versus ≥65 years) as factors and Baseline HbA1c as a continuous covariate. The last observation carried forward (LOCF) method was used to impute missing post-BL HbA1c values; the last non-missing post-BL on-treatment measurement was used to impute the missing measurement. HbA1c values obtained after hyperglycemic rescue were treated as missing and were replaced with pre-rescue values. (NCT00849017)
Timeframe: Baseline and Week 52

Change From Baseline in Body Weight at Week 156

Intervention	Percentage of HbA1c in the blood (Least Squares Mean)
Placebo	0.15
Albiglutide 30 mg	-0.70
Albiglutide 50 mg	-0.89

Change From Baseline in Body Weight at Week 52

Intervention	Kilograms (Mean)
Placebo	-2.91
Albiglutide 30 mg	-1.32
Albiglutide 50 mg	-2.24

Change From Baseline in Fasting Plasma Glucose (FPG) at Week 156

Intervention	Kilograms (Least Squares Mean)
Placebo	-0.66
Albiglutide 30 mg	-0.39
Albiglutide 50 mg	-0.86

Change From Baseline in Fasting Plasma Glucose (FPG) at Week 52

Intervention	Millimoles per liter (mmol/L) (Mean)
Placebo	-0.23
Albiglutide 30 mg	-1.31
Albiglutide 50 mg	-1.83

Change From Baseline in Postprandial Blood Glucose Profile Parameter- 4 Hour Blood Glucose AUC

Intervention	Millimoles per liter (mmol/L) (Least Squares Mean)
Placebo	1.00
Albiglutide 30 mg	-0.88
Albiglutide 50 mg	-1.38

Changes from Baseline at Week 52 in postprandial parameters after a mixed-meal (MM) tolerance test were analyzed. Post prandial blood glucose parameter analyzed was: 4 hour blood glucose area under urve AUC The AUC was determined using the trapezoidal method using measurements until 4 hours following the meal. The standardized AUC is the total AUC divided by elapsed time. Those parameters were analyzed analogous to the primary endpoint using an ANCOVA model with treatment group as a factor, and corresponding Baseline postprandial profile as a continuous covariate. This analysis used observed values excluding those obtained after hyperglycemia rescue; no missing data imputation was performed. (NCT00849017)
Timeframe: Baseline and Week 52

Change From Baseline in Postprandial Blood Glucose Profile Parameter-4 Hour C-peptide AUC

Intervention	Nanomoles/Liter (nmol/L) (Least Squares Mean)
Placebo	-0.51
Albiglutide 30 mg	-1.74
Albiglutide 50 mg	-2.05

Changes from Baseline at Week 52 in postprandial parameters after a mixed-meal (MM) tolerance test were analyzed. Post prandial blood glucose parameter analyzed was 4 hour c-peptide AUC. The AUC was determined using the trapezoidal method using measurements until 4 hours following the meal. The standardized AUC is the total AUC divided by elapsed time. Those parameters were analyzed analogous to the primary endpoint using an ANCOVA model with treatment group as a factor, and corresponding Baseline postprandial profile as a continuous covariate. This analysis used observed values excluding those obtained after hyperglycemia rescue; no missing data imputation was performed. (NCT00849017)
Timeframe: Baseline and Week 52

Time to Hyperglycemia Rescue

Intervention	Nanomoles/Liter (nmol/L) (Least Squares Mean)
Placebo	0.05
Albiglutide 30 mg Weekly	0.03
Albiglutide 50 mg Weekly	0.08

Participants who experienced persistent hyperglycemia (high blood glucose) could have qualified for hyperglycemia rescue. The conditions for hyperglycemia rescue were as follows: FPG >=280 milligrams/deciliter (mg/dL) between >=Week 2 and =250 mg/dL between >=Week 4 and =8.5% and a <=0.5% reduction from Baseline between >=Week 12 and =8.5% between >=Week 24 and =8.0% between >= Week 48 and NCT00849017)
Timeframe: From the start of study medication until the end of the treatment (up to Week 156)

Albiglutide Plasma Concentration at Weeks 8 and 24

Intervention	Weeks (Median)
Placebo	49.71
Albiglutide 30 mg	118.43
Albiglutide 50 mg	NA

Albiglutide plasma concentration data was analyzed at Week 8 pre-dose, Week 8 post dose, Week 24 pre-dose and Week 24 post-dose. All participants who received albiglutide were initiated on a 30mg weekly dosing regimen; however, beginning at Week 12, participants in the albiglutide 50 mg treatment group were uptitrated to receive albiglutide 50 mg for the remainder of the study. (NCT00849017)
Timeframe: Weeks 8 and 24

Change From Baseline in HbA1c at Weeks 104 and 156

Intervention	nanograms/milliliter (ng/mL) (Mean)
	Week 8 Pre-dose, n=85, 85	Week 8 Post-dose, n=87, 80	Week 24 Pre-dose, n=79, 74	Week 24 Post-dose, n=81, 72
Albiglutide 30 mg	1582	1900	1912	2289
Albiglutide 50 mg	1433	1759	3060	3484

Change From Baseline in Postprandial Blood Glucose Profile Parameters-4 Hour Insulin AUC and 4 Hour Proinsulin AUC

Intervention	Percentage of HbA1c in the blood (Mean)
	Week 104, n=21, 39, 42	Week 156, n=14, 30, 32
Albiglutide 30 mg	-0.93	-0.96
Albiglutide 50 mg	-1.18	-1.07
Placebo	-0.40	-0.61

Changes from Baseline at Week 52 in postprandial parameters after a mixed-meal (MM) tolerance test were analyzed. Post prandial blood glucose parameters analyzed were: 4-hour insulin AUC (4 hr Ins AUC), and 4-hour proinsulin AUC (4 hr pro-Ins AUC). The AUC was determined using the trapezoidal method using measurements until 4 hours following the meal. The standardized AUC is the total AUC divided by elapsed time. Those parameters were analyzed analogous to the primary endpoint using an ANCOVA model with treatment group as a factor, and corresponding Baseline postprandial profile as a continuous covariate. This analysis used observed values excluding those obtained after hyperglycemia rescue; no missing data imputation was performed. (NCT00849017)
Timeframe: Baseline and Week 52

Number of Participants Who Achieved Clinically Meaningful HbA1c Response Levels of <6.5%, <7%, and <7.5% at Week 156

Intervention	picomoles/Liter (pmol/L) (Least Squares Mean)
	4hr Ins AUC	4hr Pro-Ins AUC
Albiglutide 30 mg	2.9	1.9
Albiglutide 50 mg	39.9	-10.7
Placebo	49.2	1.0

The number of participants who acheieved the HbA1c treatment goal (i.e., HbA1c response levels of <6.5%, <7%, and <7.5% at Week 156) were assessed. (NCT00849017)
Timeframe: Week 156

Number of Participants Who Achieved Clinically Meaningful HbA1c Response Levels of <6.5%, <7%, and <7.5% at Week 52

Intervention	Participants (Number)
	Week 156, HbA1c <6.5%	Week 156, HbA1c <7.0%	Week 156, HbA1c <7.5%
Albiglutide 30 mg	10	18	24
Albiglutide 50 mg	11	19	29
Placebo	6	8	13

The number of participants who acheieved the HbA1c treatment goal (i.e., HbA1c response levels of <6.5%, <7%, and <7.5% at Week 52) were assessed. (NCT00849017)
Timeframe: Week 52

Change From Baseline (BL) in Glycosylated Hemoglobin (HbA1c) at Week 52

Intervention	Participants (Number)
	Week 52, HbA1c <6.5%	Week 52, HbA1c <7.0%	Week 52, HbA1c <7.5%
Albiglutide 30 mg	25	49	59
Albiglutide 50 mg	24	39	62
Placebo	10	21	34

HbA1c is a form of hemoglobin that is measured primarily to identify the average plasma glucose concentration over a 2- to 3-month period. The BL HbA1c value is defined as the last non-missing value before the start of treatment. Change from BL was calculated as the value at Week 52 minus the value at BL. Based on analysis of covariance (ANCOVA): change = treatment + BL HbA1c + prior myocardial infarction history + age category + region. The last observation carried forward (LOCF) method was used to impute missing post-BL HbA1c values; the last non-missing post-BL on-treatment measurement was used to impute the missing measurement. HbA1c values obtained after hyperglycemic rescue were treated as missing and were replaced with pre-rescue values. Nine par. with post-BL values obtained >14 days after the last dose or after hyperglycemic rescue were included in the analysis population but were not analyzed for this endpoint. (NCT00839527)
Timeframe: Baseline and Week 52

Change From Baseline in Body Weight at Week 52

Intervention	Percentage of HbA1c in the blood (Least Squares Mean)
Placebo + Metformin + Glimepiride	0.33
Pioglitazone + Metformin + Glimepiride	-0.80
Albiglutide + Metformin + Glimepiride	-0.55

The Baseline value is the last non-missing value before the start of treatment. Change from Baseline was calculated as the post-Baseline weight minus the Baseline weight. The LOCF method was used to impute missing post-Baseline weight values. Weight values obtained after hyperglycemia rescue were treated as missing and replaced with pre-rescue values. Based on ANCOVA: change = treatment + Baseline weight + Baseline HbA1c category + prior myocardial infarction history + age category + region. (NCT00839527)
Timeframe: Baseline and Week 52

Change From Baseline in Fasting Plasma Glucose (FPG) at Week 52

Intervention	Kilograms (Least Squares Mean)
Placebo + Metformin + Glimepiride	-0.40
Pioglitazone + Metformin + Glimepiride	4.43
Albiglutide + Metformin + Glimepiride	-0.42

The FPG test measures blood sugar levels after the participant has not eaten (fasted) for 12 to 14 hours. The Baseline FPG value is the last non-missing value before the start of treatment. The LOCF method was used to impute missing post-Baseline FPG values. FPG values obtained after hyperglycemia rescue were treated as missing and replaced with pre-rescue values. Change from Baseline was calculated as the post-Baseline value minus the Baseline value. Based on ANCOVA: change = treatment + Baseline FPG + Baseline HbA1c category + prior myocardial infarction history + age category + region. (NCT00839527)
Timeframe: Baseline and Week 52

Time to Hyperglycemia Rescue

Intervention	Millimoles per liter (mmol/L) (Least Squares Mean)
Placebo + Metformin + Glimepiride	0.64
Pioglitazone + Metformin + Glimepiride	-1.74
Albiglutide + Metformin + Glimepiride	-0.69

Participants who experienced persistent hyperglycemia (high blood glucose) could have qualified for hyperglycemia rescue. The conditions for hyperglycemia rescue were as follows: FPG >=280 milligrams/deciliter (mg/dL) between >=Week 2 and =250 mg/dL between >=Week 4 and =8.5% and a <=0.5% reduction from Baseline between >=Week 12 and =8.5% between >=Week 24 and =8.0% between >= Week 48 and NCT00839527)
Timeframe: From the start of study medication until the end of the treatment (up to Week 156)

Change From Baseline in Body Weight at Week 104 and Week 156

Intervention	Weeks (Median)
Placebo + Metformin + Glimepiride	49.57
Pioglitazone + Metformin + Glimepiride	NA
Albiglutide + Metformin + Glimepiride	137.71

The Baseline value is the last non-missing value before the start of treatment. Change from Baseline was calculated as the post-Baseline weight minus the Baseline weight. This analysis used observed body weight values excluding those obtained after hyperglycemia rescue; no missing data imputation was performed. (NCT00839527)
Timeframe: Baseline, Week 104, and Week 156

Change From Baseline in FPG at Week 104 and Week 156

Intervention	Kilograms (Mean)
	Week 104, n=12, 130, 104	Week 156, n=9, 90, 71
Albiglutide + Metformin + Glimepiride	-0.90	-1.53
Pioglitazone + Metformin + Glimepiride	6.28	6.52
Placebo + Metformin + Glimepiride	-2.16	-4.47

The FPG test measures blood sugar levels after the participant has not eaten (fasted) for 12 to 14 hours. The Baseline FPG value is the last non-missing value before the start of treatment. Change from Baseline was calculated as the post-Baseline value minus the Baseline value. This analysis used observed FPG values excluding those obtained after hyperglycemia rescue; no missing data imputation was performed. (NCT00839527)
Timeframe: Baseline, Week 104, and Week 156

Change From Baseline in HbA1c at Week 104 and Week 156

Intervention	Millimoles per liter (mmol/L) (Mean)
	Week 104, n=12, 128, 103	Week 156, n=9, 88, 71
Albiglutide + Metformin + Glimepiride	-0.99	-0.88
Pioglitazone + Metformin + Glimepiride	-1.98	-1.94
Placebo + Metformin + Glimepiride	0.43	-0.50

HbA1c is a form of hemoglobin that is measured primarily to identify the average plasma glucose concentration over a 2- to 3-month period. The Baseline HbA1c value is defined as the last non-missing value before the start of treatment. Change from Baseline was calculated as the post-Baseline value minus the Baseline value. This analysis used observed HbA1c values, excluding those obtained after hyperglycemia rescue; no missing data imputation was performed. (NCT00839527)
Timeframe: Baseline, Week 104, and Week 156

Number of Participants Who Achieved Clinically Meaningful HbA1c Response Levels of <6.5%, <7%, and <7.5% at Week 156

Intervention	Percentage of HbA1c in the blood (Mean)
	Week 104, n=12, 130, 104	Week 156, n=9, 89, 71
Albiglutide + Metformin + Glimepiride	-0.76	-0.46
Pioglitazone + Metformin + Glimepiride	-1.09	-0.97
Placebo + Metformin + Glimepiride	-0.32	-0.10

The number of participants who acheieved the HbA1c treatment goal (i.e., HbA1c response levels of <6.5%, <7%, and <7.5% at Week 156) was assessed. (NCT00839527)
Timeframe: Week 156

Number of Participants Who Achieved Clinically Meaningful HbA1c Response Levels of <6.5%, <7%, and <7.5% at Week 52

Intervention	Participants (Number)
	HbA1c <6.5%	HbA1c <7.0%	HbA1c <7.5%
Albiglutide + Metformin + Glimepiride	16	26	45
Pioglitazone + Metformin + Glimepiride	23	44	68
Placebo + Metformin + Glimepiride	1	3	5

The number of participants who acheieved the HbA1c treatment goal (i.e., HbA1c response levels of <6.5%, <7%, and <7.5% at Week 52) was assessed. Values were carried forward for participants who were rescued or discontinued from active treatment before Week 52. (NCT00839527)
Timeframe: Week 52

Change From Baseline (BL) in Glycosylated Hemoglobin (HbA1c) at Week 104

Intervention	Participants (Number)
	HbA1c <6.5%	HbA1c <7.0%	HbA1c <7.5%
Albiglutide + Metformin + Glimepiride	27	79	126
Pioglitazone + Metformin + Glimepiride	37	94	150
Placebo + Metformin + Glimepiride	4	10	19

HbA1c is a form of hemoglobin that is measured primarily to identify the average plasma glucose concentration over a 2- to 3-month period. The BL HbA1c value is defined as the last non-missing value before the start of treatment. Change from BL was calculated as the value at Week 104 minus the value at BL. Based on analysis of covariance (ANCOVA): change = treatment + BL HbA1c + prior myocardial infarction history + age category + region. Difference of least squares means (albiglutide - placebo, albiglutide - sitagliptin, albiglutide - glimepiride) is from the ANCOVA model. The last observation carried forward (LOCF) method was used to impute missing post-Baseline HbA1c values; the last non-missing post-BL on-treatment measurement was used to impute the missing measurement. HbA1c values obtained after hyperglycemic rescue were treated as missing and were replaced with pre-rescue values. (NCT00838903)
Timeframe: Baseline and Week 104

Change From Baseline in Body Weight at Week 104

Intervention	Percentage of HbA1c in the blood (Least Squares Mean)
Placebo Plus Metformin	0.27
Sitagliptin 100 mg Plus Metformin	-0.28
Glimepiride 2 mg Plus Metformin	-0.36
Albiglutide 30 mg Plus Metformin	-0.63

The Baseline value is the last non-missing value before the start of treatment. Change from Baseline was calculated as the post-Baseline weight minus the Baseline weight. The LOCF method was used to impute missing post-Baseline weight values. Weight values obtained after hyperglycemia rescue were treated as missing and replaced with prerescue values. Based on ANCOVA: change = treatment + Baseline weight + Baseline HbA1c category + prior myocardial infarction history + age category + region. (NCT00838903)
Timeframe: Baseline and Week 104

Change From Baseline in Body Weight at Week 156

Intervention	Kilograms (Least Squares Mean)
Placebo Plus Metformin	-1.00
Sitagliptin 100 mg Plus Metformin	-0.86
Glimepiride 2 mg Plus Metformin	1.17
Albiglutide 30 mg Plus Metformin	-1.21

Change From Baseline in Fasting Plasma Glucose (FPG) at Week 104

Intervention	Kilograms (Mean)
Placebo Plus Metformin	-3.61
Sitagliptin 100 mg Plus Metformin	-2.05
Glimepiride 2 mg Plus Metformin	0.98
Albiglutide 30 mg Plus Metformin	-2.31

The FPG test measures blood sugar levels after the participant has not eaten (fasted) for 12 to 14 hours. The Baseline FPG value is the last non-missing value before the start of treatment. The LOCF method was used to impute missing post-Baseline FPG values. FPG values obtained after hyperglycemia rescue were treated as missing and replaced with pre-rescue values. Change from Baseline was calculated as the post-Baseline value minus the Baseline value. Based on ANCOVA: change = treatment + Baseline FPG + Baseline HbA1c category + prior myocardial infarction history + age category + region. (NCT00838903)
Timeframe: Baseline and Week 104

Change From Baseline in FPG at Week 156

Intervention	Millimoles per liter (mmol/L) (Least Squares Mean)
Placebo Plus Metformin	0.55
Sitagliptin 100 mg Plus Metformin	-0.12
Glimepiride 2 mg Plus Metformin	-0.41
Albiglutide 30 mg Plus Metformin	-0.98

The FPG test measures blood sugar levels after the participant has not eaten (fasted) for 12 to 14 hours. The Baseline FPG value is the last non-missing value before the start of treatment. Change from Baseline was calculated as the post-Baseline value minus the Baseline value. This analysis used observed FPG values excluding those obtained after hyperglycemia rescue; no missing data imputation was performed. (NCT00838903)
Timeframe: Baseline and Week 156

Change From Baseline in HbA1c at Week 156

Time to Hyperglycemia Rescue

Participants who experienced persistent hyperglycemia (high blood glucose) could have qualified for hyperglycemia rescue.The conditions for hyperglycemic rescue were as follows: FPG >=280 milligrams/deciliter (mg/dL) between >=Week 2 and =250 mg/dL between >=Week 4 and =8.5% and a <=0.5% reduction from Baseline between >=Week 12 and =8.5% between >=Week 24 and =8.0% between >= Week 48 and NCT00838903)
Timeframe: From the start of study medication until the end of the treatment (up to Week 156)

Number of Participants Who Achieved Clinically Meaningful HbA1c Response Levels of <6.5%, <7%, and <7.5% at Week 104

The number of participants who achieved the HbA1c treatment goal (i.e., HbA1c response levels of <6.5%, <7%, and <7.5% at Week 52) were assessed. (NCT00838903)
Timeframe: Week 104

Number of Participants Who Achieved Clinically Meaningful HbA1c Response Levels of <6.5%, <7%, and <7.5% at Week 156

The number of participants who achieved the HbA1c treatment goal (i.e., HbA1c response levels of <6.5%, <7%, and <7.5% at Week 156) were assessed. (NCT00838903)
Timeframe: Week 156

2-hour Postload Plasma Glucose (2-h PG)

The blood sample for determining of 2-h PG, was taken two hours after the ingestion of the drink with 75 g dextrose and was evaluated by spectrophotometry method. The value was expressed on mmol/L. (NCT02370121)
Timeframe: week 12

Area Under the Curve of Glucose (AUCG)

The estimation for AUCG was calculated from parameters obtained during the 2 hours oral glucose tolerant test (OGTT) with 75 g dextrose by trapezoidal integration. The value was expressed mmol/L/min. (NCT02370121)
Timeframe: week 12

Area Under the Curve of Insulin (AUCI)

The estimation for AUCI was calculated from parameters obtained during the 2 hours oral glucose tolerant test (OGTT) with 75 g dextrose by trapezoidal integration. The value was expressed on pmol/L/min. (NCT02370121)
Timeframe: week 12

Body Mass Index (BMI)

The BMI was calculated by the square of the body height, and is universally expressed in units of kg/m2, resulting from mass in kilograms and height in metres. (NCT02370121)
Timeframe: week 12

Body Weight (BW)

The BW was evaluated after an overnight fast, through a bioimpedance digital scale results are reported in kilograms with a decimal. (NCT02370121)
Timeframe: week 12

Diastolic Blood Pressure (DBP)

The DBP was evaluated with a digital sphygmomanometer with the subject sited down on a chair after a resting period of 5 minutes on three occasions. The mean of the three measures was considered as the value of DBP. The value was expressed on mmHg. (NCT02370121)
Timeframe: week 12

Fasting Plasma Glucose (FPG)

The blood sample for determining of FPG, was taken after an overnight fast and was evaluated by spectrophotometry method. The value was expressed on mmol/L. (NCT02370121)
Timeframe: week 12

First Phase of Insulin Secretion

The first phase of insulin secretion was estimated using the Stumvoll index (1283+ 1.829 x insulin 30' - 138.7 x glucose 30' + 3.772 x insulin 0'). (NCT02370121)
Timeframe: week 12

High-density Lipoprotein Cholesterol (HDL-C)

The blood sample for determining of HDL-C, was taken after an overnight fast and was evaluated by colorimetric method. The value was expressed on mmol/L. (NCT02370121)
Timeframe: Week 12

Insulin Sensitivity

The insulin sensitivity was calculated with Matsuda index [10,000 / √glucose 0' x insulin 0') (mean glucose oral glucose tolerance test (OGTT) x mean insulin OGTT)]. (NCT02370121)
Timeframe: week 12

Low-density Lipoprotein Cholesterol (LDL-C)

The blood sample for determining of LDL-C, was taken after an overnight fast and was calculated by Friedewald formula. The value was expressed on mmol/L. (NCT02370121)
Timeframe: Week 12

Systolic Blood Pressure (SBP)

The SBP was evaluated with a digital sphygmomanometer with the subject sited down on a chair after a resting period of 5 minutes on three occasions. The mean of the three measures was considered as the value of SBP. The value was expressed on mmHg. (NCT02370121)
Timeframe: week 12

Total Cholesterol (TC)

The blood sample for determining of TC, was taken after an overnight fast and was evaluated by spectrophotometry method. The value was expressed on mmol/L. (NCT02370121)
Timeframe: week 12

Total Insulin Secretion

The total insulin secretion was calculated by the insulinogenic index (ΔABC insulin / ΔABC glucose). (NCT02370121)
Timeframe: Week 12

Triglycerides (TGs)

The blood sample for determining of TGs, was taken after an overnight fast and was evaluated by spectrophotometry method. The value was expressed on mmol/L. (NCT02370121)
Timeframe: week 12

Very-low Density Lipoprotein (VLDL)

The blood sample for determining the VLDL, was taken after an overnight fast and was calculated as triglycerides/5. The value was expressed on mmol/L. (NCT02370121)
Timeframe: week 12

Waist Circumference (WC)

The WC was evaluated after an overnight fast with a flexible tape in the midpoint between the lowest rib and the iliac crest and is expressed in centimeters. (NCT02370121)
Timeframe: Week 12

Body Weight Change From Baseline

"Change from baseline in body weight after 24 weeks.~Note that adjusted means are provided." (NCT01210001)
Timeframe: Baseline and 24 weeks

Fasting Plasma Glucose (FPG) Change From Baseline

"Change from baseline in fasting plasma glucose (FPG) after 24 weeks of treatment.~Note that adjusted means are provided." (NCT01210001)
Timeframe: Baseline and 24 weeks

HbA1c Change From Baseline

"Change From Baseline in HbA1c after 24 weeks.~Note that adjusted means are provided." (NCT01210001)
Timeframe: Baseline and 24 weeks

HbA1c Change From Baseline for Pio and Met Background Medication Patients

"Change From Baseline in HbA1c after 24 weeks for patients with pioglitazone (pio) and metformin (met) background medication only.~Note that adjusted means are provided." (NCT01210001)
Timeframe: Baseline and 24 weeks

Hypoglycaemic Events

Number of patients with hypoglycaemic events, as reported as adverse events. (NCT01210001)
Timeframe: From first drug administration until 7 days after last intake of study drug, up to 256 days

The Change in Levels of High Sensitivity C-reactive Protein From Baseline to 16 Weeks in the Sitagliptin and Gliclazide Arms.

High sensitivity C-reactive protein (range 0 - no maximum) (NCT01991197)
Timeframe: 16 weeks

The Change in Levels of Serum Glucose From Baseline to 16 Weeks in the Sitagliptin and Gliclazide Arms.

The change in glucose from baseline to 16 weeks (NCT01991197)
Timeframe: 16 weeks

The Change in Levels of Systolic Blood Pressure From Baseline to 16 Weeks in the Sitagliptin and Gliclazide Arms.

The change in systolic blood pressure from baseline to 16 weeks measured in kg (NCT01991197)
Timeframe: 16 weeks

The Change in Levels of Total Cholesterol From Baseline to 16 Weeks in the Sitagliptin and Gliclazide Arms.

The change in total cholesterol from baseline to 16 weeks (NCT01991197)
Timeframe: 16 weeks

The Change in PASI From Baseline to 32 Weeks in Psoriasis Patients With Type 2 Diabetes Treated With Sitagliptin Compared to Patients Treated With Gliclazide.

Psoriasis area and severity index 0-72, higher score worse outcome (NCT01991197)
Timeframe: baseline and 32 weeks

The Change in the Psoriasis Area and Severity Index (PASI) From Baseline to 16 Weeks in Psoriasis Patients With Type 2 Diabetes Treated With Sitagliptin Compared to Patients Treated With Gliclazide.

Psoriasis area and severity index (0-72), higher scores worse outcome (NCT01991197)
Timeframe: 16 weeks

The Change in Weight From Baseline to 16 Weeks in the Sitagliptin and Gliclazide Arms.

The change in weight from baseline to 16 weeks measured in kg (NCT01991197)
Timeframe: 16 weeks

The Effect of Treatment With Sitagliptin and With Gliclazide From Baseline to 16 Weeks on the Change in Dipeptidyl Peptidase-4 Levels in the Skin (in a Sub-group of Participants Willing to Undergo Skin Biopsies).

Dipeptidyl peptidase-4 levels levels in skin (0-no maximum) (NCT01991197)
Timeframe: 16 weeks

The Effect of Treatment With Sitagliptin and With Gliclazide From Baseline to 16 Weeks on the Change in Interleukin-17 Levels in the Skin (in a Sub-group of Participants Willing to Undergo Skin Biopsies).

The Effects of Treatment With Sitagliptin and Treatment With Gliclazide From Baseline to 16 Weeks on Serum Levels Interleukin-17.

"Secondary outcomes:~The change in serum concentrations of the cytokine interleukin-17 (IL-17) Range: 0-no maximum" (NCT01991197)
Timeframe: 16 weeks

The Effects of Treatment With Sitagliptin and Treatment With Gliclazide From Baseline to 16 Weeks on Serum Levels Interleukin-23.

"Secondary outcomes:~The change in serum concentrations of the cytokine interleukin-23 (IL-23) Range: 0-no maximum" (NCT01991197)
Timeframe: 16 weeks

The Effects of Treatment With Sitagliptin and Treatment With Gliclazide on the Change in Serum Leptin From Baseline to 16 Weeks.

"Secondary outcomes:~The change in serum concentrations of the adipokine leptin Range: 0-no maximum" (NCT01991197)
Timeframe: 16 weeks

The Effects of Treatment With Sitagliptin and Treatment With Gliclazide on the Serum Cytokine Tumour Necrosis Factor Alpha.

"Secondary outcomes:~The change in serum concentrations of the cytokines tumour necrosis factor alpha (TNFα) Range: 0-no maximum" (NCT01991197)
Timeframe: 16 weeks

The Number of Patricipants in the Sitagliptin and Gliclazide Arms With Adverse Events at 32 Weeks.

"Dosage: Sitagliptin: 100mg daily, or 50mg daily for participants with moderate kidney disease Gliclazide: 80-320 mg daily.~Secondary outcomes: the number participants with adverse events." (NCT01991197)
Timeframe: 32 weeks

The Change in Quality of Life Scores From Baseline to 16 Weeks in the Sitagliptin and Gliclazide Arms.

"Dermatology life quality index (a skin related quality of life measure) (0-10), higher score worse outcome EQ-5D Euroqol 5 item quality of life index comprising 5 dimensions mobility, self-care, usual activities, pain, anxiety. An index can be derived from these 5 dimensions by conversion with a table of scores. The maximum score of 1 indicates the best health state and minimum score indicating the worst health outcome -0.594.~HADS Hospital anxiety and depression scale 0-16 for anxiety and 0-16 for depression, higher score worse outcome HAQ-8 Stanford 8 item disability scale. Scoring is from 0 (without any difficulty) to 3 (unable to do). The 8 scores from the 8 sections are summed and divided by 8. The result is the disability index (range 0-3 with 25 possible values). A" (NCT01991197)
Timeframe: 16 weeks

The Effects of Treatment With Sitagliptin and Treatment With Gliclazide on Other Efficacy Endpoints.

"Secondary outcomes:~d. number or participants who acheived a greater than 50% reduction in PASI from baseline (PASI-50); e. number of participants who achieved PASI-75 and PASI-90." (NCT01991197)
Timeframe: 16 weeks

Effects of Pioglitazone on 24h Blood Pressure Control

24 hour blood pressure measurements were performed after each treatment/diet phase (NCT01090752)
Timeframe: march 2009

Effects of Pioglitazone on Renal Hemodynamics

At the end of each treatment diet phase, renal clearances were performed for the determination of GFR and RBF (NCT01090752)
Timeframe: 2008

Effects of Pioglitazone on Sodium and Lithium Clearances

At the end of each treatment and diet phase, 24 urine collections were collected for the determination of sodium and lithium clearances (NCT01090752)
Timeframe: 2007

Change in Body Weight

Change in body weight following 30 weeks of therapy (i.e., body weight at week 30 minus body weight at baseline) (NCT00765817)
Timeframe: baseline and 30 weeks

Change in Daily Insulin Dose

Change in daily insulin dose following 30 weeks of therapy (i.e., daily insulin dose at week 30 minus daily insulin dose at baseline) (NCT00765817)
Timeframe: baseline and 30 weeks

Change in Daily Insulin Dose (on a Per Body Weight Basis)

Change in daily insulin dose per kilogram (kg) following 30 weeks of therapy (i.e., daily insulin dose per kg at week 30 minus daily insulin dose per kg at baseline) (NCT00765817)
Timeframe: baseline and 30 weeks

Change in Diastolic Blood Pressure (DBP)

Change in DBP following 30 weeks of therapy (i.e., DBP at week 30 minus DBP at baseline) (NCT00765817)
Timeframe: baseline and 30 weeks

Change in Fasting Serum Glucose

Change in fasting serum glucose following 30 weeks of therapy (i.e., fasting serum glucose at week 30 minus fasting serum glucose at baseline) (NCT00765817)
Timeframe: baseline and 30 weeks

Change in Glycosylated Hemoglobin (HbA1c)

Change in HbA1c from baseline following 30 weeks of therapy (i.e., HbA1c at week 30 minus HbA1c at baseline). Unit of measure is percent of hemoglobin that is glycosylated. (NCT00765817)
Timeframe: baseline and 30 weeks

Change in High Density Lipoprotein (HDL) Cholesterol

Change in HDL cholesterol following 30 weeks of therapy (i.e., HDL cholesterol at week 30 minus HDL cholesterol at baseline) (NCT00765817)
Timeframe: baseline and 30 weeks

Change in Low Density Lipoprotein (LDL) Cholesterol

Change in LDL cholesterol following 30 weeks of therapy (i.e., LDL cholesterol at week 30 minus LDL cholesterol at baseline) (NCT00765817)
Timeframe: baseline and 30 weeks

Change in Systolic Blood Pressure (SBP)

Change in SBP following 30 weeks of therapy (i.e., SBP at week 30 minus SBP at baseline) (NCT00765817)
Timeframe: baseline and 30 weeks

Change in Total Cholesterol

Change in total cholesterol following 30 weeks of therapy (i.e., total cholesterol at week 30 minus total cholesterol at baseline) (NCT00765817)
Timeframe: baseline and 30 weeks

Change in Triglycerides

Change in triglycerides following 30 weeks of therapy (i.e., triglycerides at week 30 minus triglycerides at baseline) (NCT00765817)
Timeframe: baseline and 30 weeks

Change in Waist Circumference

Change in waist circumference following 30 weeks of therapy (i.e., waist circumference at week 30 minus waist circumference at baseline) (NCT00765817)
Timeframe: baseline and 30 weeks

Minor Hypoglycemia Rate Per Year

Number of minor hypoglycemia events experienced per subject per year. Minor hypoglycemia was defined as any time a subject felt he or she was experiencing a sign or symptom associated with hypoglycemia that was either self-treated by the subject or resolved on its own and had a concurrent finger stick blood glucose <3.0 mmol/L (54 mg/dL). (NCT00765817)
Timeframe: baseline and weeks 2, 4, 6, 8, 10, 14, 18, 22, 26, and 30

Percentage of Patients Achieving HbA1c <=6.5%

Percentage of patients in each arm who had HbA1c >6.5% at baseline and had HbA1c <=6.5% at week 30 (percentage = [number of subjects with HbA1c <=6.5% at week 30 divided by number of subjects with HbA1c >6.5% at baseline] * 100%). (NCT00765817)
Timeframe: baseline and 30 weeks

Percentage of Patients Achieving HbA1c <=7%

Percentage of patients in each arm who had HbA1c >7% at baseline and had HbA1c <=7% at week 30 (percentage = [number of subjects with HbA1c <=7% at week 30 divided by number of subjects with HbA1c >7% at baseline] * 100%). (NCT00765817)
Timeframe: baseline and 30 weeks

Percentage of Subjects Experiencing Minor Hypoglycemia

Percentage of subjects in each arm experiencing at least one episode of minor hypoglycemia at any point during the study. Minor hypoglycemia was defined as any time a subject felt he or she was experiencing a sign or symptom associated with hypoglycemia that was either self-treated by the subject or resolved on its own and had a concurrent finger stick blood glucose <3.0 mmol/L (54 mg/dL). (NCT00765817)
Timeframe: baseline and weeks 2, 4, 6, 8, 10, 14, 18, 22, 26, and 30

Change in 7-point Self-monitored Blood Glucose (SMBG) Profile

Change in 7-point (pre-breakfast, 2 hour post-breakfast, pre-lunch, 2 hour post-lunch, pre-dinner, 2 hour post-dinner, 0300 hours) SMBG profile from baseline to week 30 (change = blood glucose value at week 30 minus blood glucose value at baseline) (NCT00765817)
Timeframe: baseline and 30 weeks

Hepatic Fat

The effect of exenatide and pioglitazone on liver fat content after one year of treatment in patients with type 2 diabetes. (NCT01432405)
Timeframe: one year

Plasma Adipocytokines

the effect of the intervention on plasma adiponectin levels. (NCT01432405)
Timeframe: one year

Alanine Aminotransferase (ALT) at Week 12.

The ALT hepatic transaminase levels are going to be measured at week 12 with standardized techniques. (NCT02113241)
Timeframe: Week 12.

Aspartate Aminotransferase (AST) at Week 12.

The hepatic transaminase AST will be evaluated with standardized methods at week 12 (NCT02113241)
Timeframe: Week 12

AUC of Glucose at Week 12.

The AUC of glucose will be calculated from the glucose values obtained from the minuted oral glucose tolerance curve at week 12 (NCT02113241)
Timeframe: Week 12

AUC of Insulin at Week 12.

The AUC will be calculated from the insulin values obtained from the minuted oral glucose tolerance curve at week 12 (NCT02113241)
Timeframe: Week 12

Body Mass Index at Week 12

The Body Mass index it's going to be calculated at week 12 with the Quetelet index. (NCT02113241)
Timeframe: Week 12

Body Weight at Week 12.

The weight it's going to be measured at week 12 with a bioimpedance balance. (NCT02113241)
Timeframe: Week 12

Creatinine at Week 12.

The creatinine levels are going to be measured at week 12 with standardized techniques. (NCT02113241)
Timeframe: Week 12.

Diastolic Blood Pressure at Week 12.

The diastolic blood pressure is going to be evaluated at week 12 with a digital sphygmomanometer. (NCT02113241)
Timeframe: Week 12

Fat Mass at Week 12.

The fat mass is going to be evaluated at week 12 through bioimpedance. (NCT02113241)
Timeframe: Week 12

Glucose at Minute 120 at Week 12.

The glucose at minute 120 is going to be evaluated at week 12 during a minuted oral glucose tolerance curve (NCT02113241)
Timeframe: Week 12

Glucose at Minute 30 at Week 12.

The glucose at minute 30 is going to be evaluated at week 12 during a minuted oral glucose tolerance curve (NCT02113241)
Timeframe: Week 12

Glucose at Minute 60 at Week 12.

The glucose at minute 60 is going to be evaluated at week 12 during a minuted oral glucose tolerance curve (NCT02113241)
Timeframe: Week 12

Glucose at Minute 90 at Week 12.

The glucose at minute 90 is going to be evaluated at week 12 during a minuted oral glucose tolerance curve (NCT02113241)
Timeframe: Week 12

Glucose Levels at Minute 0 at Week 12.

The fasting glucose (0') levels are going to be evaluated at week 12 with enzymatic/colorimetric techniques. (NCT02113241)
Timeframe: Week 12

High Density Lipoprotein (c-HDL) Levels at Week 12.

The c-HDL levels are going to be evaluated at week 12 with enzymatic/colorimetric techniques. (NCT02113241)
Timeframe: Week 12

Insulinogenic Index (Total Insulin Secretion) at Week 12.

"The insulinogenic index is a ratio that relates enhancement of circulating insulin to the magnitude of the corresponding glycemic stimulus.~Total insulin secretion was calculated with the insulinogenic index (ΔAUC insulin/ΔAUC glucose), the entered values reflect the total insulin secretion at week 12." (NCT02113241)
Timeframe: Week 12

Low Density Lipoproteins (c-LDL) at Week 12

The c-LDL levels are going to be measured at week 12 with standardized techniques. (NCT02113241)
Timeframe: Week 12

Matsuda Index (Total Insulin Sensitivity) at Week 12.

Matsuda Index value is used to indicate insulin resistance on diabetes. Insulin sensitivity was calculated with Matsuda index [10,000 / √glucose 0' x insulin 0') (mean glucose oral glucose tolerance test (OGTT) x mean insulin OGTT)]. The entered values reflect the insulin sensitivity at week 12. (NCT02113241)
Timeframe: Week 12

Stumvoll Index (First Phase of Insulin Secretion) at Week 12.

"Human studies support the critical physiologic role of the first-phase of insulin secretion in the maintenance of postmeal glucose homeostasis.~First phase of insulin secretion was estimated using the Stumvoll index (1283+ 1.829 x insulin 30' - 138.7 x glucose 30' + 3.772 x insulin 0'), the entered values reflect the frst phase of insulin secretion at week 12." (NCT02113241)
Timeframe: Week 12

Systolic Blood Pressure at Week 12.

The systolic blood pressure is going to be evaluated at week 12 with a digital sphygmomanometer. (NCT02113241)
Timeframe: Week 12

Total Cholesterol at Week 12

The total cholesterol will be estimated by standardized techniques at week 12. (NCT02113241)
Timeframe: Week 12

Triglycerides Levels at Week 12.

The triglycerides levels are going to be evaluated at week 12 with enzymatic-colorimetric techniques. (NCT02113241)
Timeframe: Week 12

Uric Acid at Week 12.

The uric acid levels are going to be measured at week 12 with standardized techniques. (NCT02113241)
Timeframe: Week 12.

Waist Circumference at Week 12.

The waist circumference is going to be evaluated at week 12 with a flexible tape with standardized techniques. (NCT02113241)
Timeframe: Week 12

Adjusted Mean Change From Baseline in 120-minute Post-challenge Plasma Glucose (PPG) (mg/dL) at Week 24 (Last Observation Carried Forward [LOCF])

Secondary endpoints were tested using sequential testing procedure and are presented in hierarchical order. In post oral glucose tolerance test (OGTT), glucose was measured as milligrams per deciliter(mg/dL) by a central laboratory. Baseline was defined as the last assessment prior to the start date and time of the first dose of the double-blind study medication. In cases where time of the first dose or time of the assessment was not available, baseline was defined as the last assessment on or prior to the date of the first dose of the double-blind study medication. PPG measurements were obtained on Day 1 and week 24 in the double-blind period. (NCT00683878)
Timeframe: From Baseline to Week 24

Adjusted Mean Change From Baseline in Fasting Plasma Glucose (FPG) at Week 24 (Last Observation Carried Forward [LOCF])

Secondary endpoints were tested using sequential testing procedure and are presented in hierarchical order. Fasting plasma glucose was measured as milligrams per deciliter(mg/dL) by a central laboratory. Baseline was defined as the last assessment prior to the start date and time of the first dose of the double-blind study medication. In cases where time of the first dose or time of the assessment was not available, baseline was defined as the last assessment on or prior to the date of the first dose of the double-blind study medication. FPG measurements were obtained during the qualification and lead-in periods and on Day 1 and Weeks 1, 2, 4, 8, 12, 16, 20, and 24 in the double-blind period. (NCT00683878)
Timeframe: From Baseline to Week 24

Adjusted Mean Change From Baseline in Hemoglobin A1C (HbA1c) at Week 24 (Last Observation Carried Forward [LOCF])

HbA1c was measured as percent of hemoglobin by a central laboratory. Data after rescue medication was excluded from this analysis. Baseline was defined as the last assessment prior to the start date and time of the first dose of the double-blind study medication. In cases where time of the first dose or time of the assessment was not available, baseline was defined as the last assessment on or prior to the date of the first dose of the double-blind study medication. HbA1c measurements were obtained during the qualification and lead-in periods and on Day 1 and Weeks 4, 8, 12, 16, 20, and 24 in the double-blind period. (NCT00683878)
Timeframe: From Baseline to Week 24

Adjusted Mean Change From Baseline in Total Body Weight (kg) Among Subjects With Baseline Body Mass Index (BMI) ≥ 27 kg/m^2 at Week 24 (Last Observation Carried Forward [LOCF])

Secondary endpoints were tested using sequential testing procedure and are presented in hierarchical order. Adjusted mean change from baseline in total body weight among subjects with baseline body mass index (BMI) ≥ 27 kg/m^2 at Week 24 (or the last postbaseline measurement prior to Week 24 if no Week 24 assessment was available was determined. Data after rescue medication was excluded from this analysis. Baseline was defined as the last assessment prior to the start date and time of the first dose of the double-blind study medication. In cases where time of the first dose or time of the assessment was not available, baseline was defined as the last assessment on or prior to the date of the first dose of the double-blind study medication. Body weight measurements were obtained during the qualification and lead-in periods and on Day 1 and Weeks 1, 2, 4, 8, 12, 16, 20, and 24 of the double-blind period. (NCT00683878)
Timeframe: From Baseline to Week 24

Adjusted Mean Change From Baseline in Total Body Weight (kg) at Week 24 (Last Observation Carried Forward [LOCF])

Secondary endpoints were tested using sequential testing procedure and are presented in hierarchical order. Adjusted mean change from baseline in total body weight at Week 24 (or the last postbaseline measurement prior to Week 24 if no Week 24 assessment was available was determined. Data after rescue medication was excluded from this analysis. Baseline was defined as the last assessment prior to the start date and time of the first dose of the double-blind study medication. In cases where time of the first dose or time of the assessment was not available, baseline was defined as the last assessment on or prior to the date of the first dose of the double-blind study medication. Body weight measurements were obtained during the qualification and lead-in periods and on Day 1 and Weeks 1, 2, 4, 8, 12, 16, 20, and 24 of the double-blind period. (NCT00683878)
Timeframe: From Baseline to Week 24

Adjusted Mean Change From Baseline in Waist Circumference (cm) at Week 24 (Last Observation Carried Forward [LOCF])

Secondary endpoints were tested using sequential testing procedure and are presented in hierarchical order. Adjusted mean change from baseline in waist circumference at Week 24 (or the last postbaseline measurement prior to Week 24 if no Week 24 assessment was available was determined. Data after rescue medication was excluded from this analysis. Baseline was defined as the last assessment prior to the start date and time of the first dose of the double-blind study medication. In cases where time of the first dose or time of the assessment was not available, baseline was defined as the last assessment on or prior to the date of the first dose of the double-blind study medication. Waist circumference measurements were obtained during the qualification and lead-in periods and on Day 1 and Week 24 of the double-blind period. (NCT00683878)
Timeframe: From Baseline to Week 24

Percentage of Participants Achieving a Therapeutic Glycemic Response (Hemoglobin A1c [HbA1C]) <7.0% at Week 24 (Last Observation Carried Forward [LOCF])

Secondary endpoints were tested using sequential testing procedure and are presented in hierarchical order. Percent adjusted for baseline HbA1c. Therapeutic glycemic response is defined as HbA1c <7.0%. Data after rescue medication was excluded from this analysis. HbA1c was measured as a percent of hemoglobin. Mean and standard error for percentage of participants were estimated by modified logistic regression model. (NCT00683878)
Timeframe: From Baseline to Week 24

Comparison of Changes in Fasting Serum Glucose (FSG)With Pioglitazone and Metformin

Response rate was defined by ≥10% decrease of FSG or/and ≥1% decrease of HbA1c from the baseline values after 3 months treatment.48 responded to pioglitazone and 32 responded to metformin. (NCT01589445)
Timeframe: 3 months for each drug

Comparison of Changes in Fasting Serum Insulin (FSI)With Pioglitazone and Metformin

Comparison of Changes in Glycosylated Hemoglobin (HbA1c)With Pioglitazone and Metformin

Comparison of Changes in HOMA Percent B and HOMA Percent S With Pioglitazone and Metformin

"Response rate was defined by ≥10% decrease of FSG or/and ≥1% decrease of HbA1c from the baseline values after 3 months treatment.48 responded to pioglitazone and 32 responded to metformin.~Analysis 1: Homeostatic Model Assessment of Beta cell function(HOMA percent B) Analysis 2: Homeostatic Model Assessment of Insulin Sensitivity (Homa percent S)" (NCT01589445)
Timeframe: 3 months for each drug

Comparison of Changes in Insulin Levels (HOMA IR,QUICKI) With Pioglitazone and Metformin

"Response rate was defined by ≥10% decrease of FSG or/and ≥1% decrease of HbA1c from the baseline values after 3 months treatment.48 responded to pioglitazone and 32 responded to metformin.~Analysis 1: Homeostasis Model Assessment Insulin Resistance(HOMA IR) Analysis 2: Quantitative Insulin sensitivity Check Index(QUICKI)" (NCT01589445)
Timeframe: 3 months for each drug

Comparison of Changes in Lipid Profiles With Pioglitazone and Metformin

"Response rate was defined by ≥10% decrease of FSG or/and ≥1% decrease of HbA1c from the baseline values after 3 months treatment.48 responded to pioglitazone and 32 responded to metformin.~Analysis 1:Total Cholesterol(TC) Analysis 2:Triglyceride(TG) Analysis 3:High Density Lipoprotein(HDL) Analysis 4:Low Density Lipoprotein(LDL)" (NCT01589445)
Timeframe: 3 months for each drug

Cholesterol Efflux Capacity of HDL

The ability of serum HDL to remove cholesterol from cultured cells will be assessed as an in vitro method to evaluate a functional changes in HDL mediated by changes due to pioglitazone treatment. Cells were incubated with 2% serum from each study subject diluted in culture medium and incubations were performed for a total of 4 hours. Cholesterol efflux was calculated as the percent of cholesterol removed from the cells and appearing in the culture medium normalized to a reference serum pool as described in detail by de la Llera-Moya et al (de la Llera-Moya M, Drazul-Schrader D, Asztalos BF, Cuchel M, Rader DJ, Rothblat GH. The ability to promote efflux via ABCA1 determines the capacity of serum specimens with similar high-density lipoprotein cholesterol to remove cholesterol from macrophages. Arterioscler Thromb Vasc Biol. 2010 Apr;30(4):796-801. doi: 10.1161/ATVBAHA.109.199158. PMID: 20075420). (NCT01156597)
Timeframe: 24 weeks

HDL Apolipoprotein Levels at Study End-point

Lipoproteins will be isolated and analyzed using the gradient ultracentrifugation-high pressure liquid chromatography technique to isolate very low-density lipoprotein (VLDL), intermediate density lipoprotein (IDL), LDL, and high density lipoprotein (HDL) subfractions. Protein and lipid compositions of HDL is determined (NCT01156597)
Timeframe: 24 weeks

Increased HDL-Cholesterol and Decreased Triglycerides

"The primary endpoint will be increased high density lipoprotein cholesterol and decreased triglycerides measured as the difference after 12 or 24 weeks of treatment from baseline levels. The data are expressed as the percent change from the baseline value and calculated using he equation:~Change=[100%*(Endpoint value - Baseline Value)/Baseline Value]" (NCT01156597)
Timeframe: 24 weeks

Intervention	Millimoles per liter (mmol/L) (Mean)
Placebo Plus Metformin	-0.11
Sitagliptin 100 mg Plus Metformin	-0.50
Glimepiride 2 mg Plus Metformin	-0.71
Albiglutide 30 mg Plus Metformin	-1.30

Intervention	Weeks (Median)
Placebo Plus Metformin	67.71
Sitagliptin 100 mg Plus Metformin	NA
Glimepiride 2 mg Plus Metformin	NA
Albiglutide 30 mg Plus Metformin	NA

Intervention	score on a scale (Median)
	DLQI	HAQ-8	HADS Anxiety	HADS Depression	EQ-5D
Gliclazide	-1.0	0.0	0	0	-0.2
Sitagliptin	0.0	0.0	-1	0	0

Intervention	mmHg (Mean)
Pioglitazone Low Salt/High Salt	128
Placebo Low Salt/High Salt	129

Intervention	ml/min/1.73m2 (Mean)
Pioglitazone Low Salt/High Salt	68.0
Placebo Low Salt/High Salt	62.4

Intervention	ml/min (Mean)
Pioglitazone Low Salt/High Salt	1.05
Placebo Low Salt/High Salt	1.18

Intervention	mmol/L (Least Squares Mean)
	Pre-breakfast: baseline	Pre-breakfast: change at week 30	2 hour post-breakfast: baseline	2 hour post-breakfast: change at week 30	Pre-lunch: baseline	Pre-lunch: change at week 30	2 hour post-lunch: baseline	2 hour post-lunch: change at week 30	Pre-dinner: baseline	Pre-dinner: change at week 30	2 hour post-dinner: baseline	2 hour post-dinner: change at week 30	0300: baseline	0300: change at week 30
Exenatide Arm	7.89	-1.58	10.89	-3.56	8.95	-2.23	11.35	-2.74	9.85	-2.25	12.03	-3.87	8.95	-2.27
Placebo Arm	8.27	-1.48	11.82	-1.72	9.77	-1.15	11.70	-1.38	9.99	-1.33	11.86	-1.34	9.20	-1.48

Intervention	mg/dL (Mean)
PLACEBO + Pioglitazone	-14.1
Dapagliflozin 5MG + Pioglitazone	-65.1
Dapagliflozin 10MG + Pioglitazone	-67.5

Intervention	mg/dL (Mean)
PLACEBO + Pioglitazone	-5.5
Dapagliflozin 5MG + Pioglitazone	-24.9
Dapagliflozin 10MG + Pioglitazone	-29.6

Intervention	kg (Mean)
PLACEBO + Pioglitazone	1.83
Dapagliflozin 5MG + Pioglitazone	0.26
Dapagliflozin 10MG + Pioglitazone	-0.07

Intervention	kg (Mean)
PLACEBO + Pioglitazone	1.64
Dapagliflozin 5MG + Pioglitazone	0.09
Dapagliflozin 10MG + Pioglitazone	-0.14

Intervention	Percentage of participants (Mean)
PLACEBO + Pioglitazone	22.4
Dapagliflozin 5MG + Pioglitazone	32.5
Dapagliflozin 10MG + Pioglitazone	38.8

Intervention	mmol/l (Mean)
	Baseline FSG	3rd Month FSG
Metformin ( 002 Group)	6.2	6.5
Pioglitazone (001 Group)	6.9	5.4

Intervention	μU/ml (Mean)
	Baseline FSI	3rd month FSI
Metformin ( 002 Group)	13.0	13.9
Pioglitazone (001 Group)	16.2	12.3

Intervention	percentage (Mean)
	Baseline HbA1c	3rd month HbA1c
Metformin ( 002 Group)	7.8	7.0
Pioglitazone (001 Group)	7.3	6.7

Intervention	percentage (Mean)
	Baseline HOMA percent beta cells function	3rd month HOMA percent beta cells function	Baseline HOMA percent sensitivity	3rd month HOMA percent sensitivity
Metformin ( 002 Group)	109.3	116.0	76.2	67.2
Pioglitazone (001 Group)	118.9	132.3	51.1	69.3

Intervention	Score on a scale ( SI unit) (Mean)
	Baseline QUICKI	3rd month QUICKI	Baseline HOMA IR	3rd month HOMA IR
Metformin ( 002 Group)	0.57	0.54	3.7	4.3
Pioglitazone (001 Group)	0.52	0.59	5.1	2.9

Intervention	mg/dl (Mean)
	Baseline TC	3rd month TC	Baseline TG	3rd month TG	Baseline HDL	3rd month HDL	Baseline LDL	3rd month LDL
Metformin (002 Group)	193.0	177.0	166.0	175.0	34.4	34.7	125.6	112.0
Pioglitazone (001 Group)	182.0	178	183	195	33	33.2	112.8	105.5

Intervention	mg/dL (Mean)
	HDL-apoAI at end point	HDL-apoAII at end point	HDL-apoCI at end point	HDL-apoCII at end point	HDL-apoCIII at end point	HDL-apoM at end point
Comparator Group	65.7	22.6	8.4	2.8	12.5	0.43
Pioglitazone Group	65.0	26.6	10.9	3.5	11.8	0.62

Intervention	% Change (Mean)
	% Change in HDL cholesterol at 12 weeks	% Change in HDL cholesterol at 24 weeks	% Change in triglycerides at 12 weeks	% Change in triglycerides at 24 weeks
Comparator Group	2.7	-1.5	7.4	19.7
Pioglitazone Group	7.9	15.7	-10.9	-15.4

Article	Year
Impact of pharmacological interventions on anthropometric indices in women with polycystic ovary syndrome: A systematic review and meta-analysis of randomized controlled trials. Clinical endocrinology, 2022, Volume: 96, Issue:6 Topics: Acarbose; Body Weight; Female; Humans; Hypoglycemic Agents; Metformin; Orlistat; Pioglitazone; Polyc	2022
Diabetes drugs for nonalcoholic fatty liver disease: a systematic review. Systematic reviews, 2019, 11-29, Volume: 8, Issue:1 Topics: Blood Glucose; Body Weight; Exenatide; Glycated Hemoglobin; Humans; Hypoglycemic Agents; Liraglutide	2019
Efficacy of Various Hypoglycemic Agents in the Treatment of Patients With Nonalcoholic Liver Disease With or Without Diabetes： A Network Meta-Analysis. Frontiers in endocrinology, 2021, Volume: 12 Topics: Alanine Transaminase; Aspartate Aminotransferases; Bayes Theorem; Blood Glucose; Body Mass Index; Bo	2021
Nonalcoholic Fatty Liver Disease and Obesity Treatment. Current obesity reports, 2019, Volume: 8, Issue:3 Topics: Bariatric Surgery; Body Weight; Diet; Exercise; Glucagon-Like Peptide 1; Humans; Inflammation; Insul	2019
Gender-specific risk factors for gout: a systematic review of cohort studies. Advances in rheumatology (London, England), 2019, 06-24, Volume: 59, Issue:1 Topics: Age Factors; Animals; Body Size; Body Weight; Cohort Studies; Diabetes Complications; Diet; Diuretic	2019
What are the preferred strategies for control of glycaemic variability in patients with type 2 diabetes mellitus? Diabetes, obesity & metabolism, 2013, Volume: 15 Suppl 2 Topics: Blood Glucose; Body Weight; Diabetes Mellitus, Type 2; Diet, Reducing; Dipeptidyl-Peptidase IV Inhib	2013
Beneficial effect of lixisenatide after 76 weeks of treatment in patients with type 2 diabetes mellitus: A meta-analysis from the GetGoal programme. Diabetes, obesity & metabolism, 2017, Volume: 19, Issue:2 Topics: Adult; Aged; Blood Glucose; Body Weight; Diabetes Mellitus, Type 2; Drug Therapy, Combination; Femal	2017
Combination therapy with DPP-4 inhibitors and pioglitazone in type 2 diabetes: theoretical consideration and therapeutic potential. Vascular health and risk management, 2008, Volume: 4, Issue:6 Topics: Adamantane; Blood Glucose; Body Weight; Clinical Trials as Topic; Diabetes Mellitus, Type 2; Dipepti	2008
Adding pioglitazone to insulin containing regimens in type 2 diabetes: systematic review and meta-analysis. PloS one, 2009, Jul-01, Volume: 4, Issue:7 Topics: Blood Glucose; Body Weight; Diabetes Mellitus, Type 2; Drug Therapy, Combination; Humans; Hypoglycem	2009
Effects of pioglitazone and rosiglitazone combined with metformin on body weight in people with diabetes. Diabetes, obesity & metabolism, 2009, Volume: 11, Issue:12 Topics: Blood Glucose; Body Weight; Diabetes Mellitus, Type 2; Drug Therapy, Combination; Female; Humans; Hy	2009
Effects of thiazolidinediones on polycystic ovary syndrome: a meta-analysis of randomized placebo-controlled trials. Advances in therapy, 2012, Volume: 29, Issue:9 Topics: Androgens; Blood Glucose; Body Weight; Female; Humans; Insulin; Insulin Resistance; Pioglitazone; Po	2012
A meta-analysis comparing the effect of thiazolidinediones on cardiovascular risk factors. Archives of internal medicine, 2004, Oct-25, Volume: 164, Issue:19 Topics: Blood Glucose; Blood Pressure; Body Weight; Cardiovascular Diseases; Diabetes Mellitus, Type 2; Glyc	2004
Pioglitazone elicits long-term improvements in insulin sensitivity in patients with type 2 diabetes: comparisons with gliclazide-based regimens. Diabetologia, 2005, Volume: 48, Issue:3 Topics: Adult; Aged; Blood Glucose; Body Mass Index; Body Weight; Diabetes Mellitus, Type 2; Double-Blind Me	2005
Pioglitazone: an antidiabetic drug with cardiovascular therapeutic effects. Expert review of cardiovascular therapy, 2006, Volume: 4, Issue:4 Topics: Body Weight; Cardiovascular Diseases; Cardiovascular System; Diabetes Mellitus; Diabetic Angiopathie	2006
Oral antidiabetic drugs: bioavailability assessment of fixed-dose combination tablets of pioglitazone and metformin. Effect of body weight, gender, and race on systemic exposures of each drug. Journal of clinical pharmacology, 2007, Volume: 47, Issue:1 Topics: Administration, Oral; Adult; Area Under Curve; Biological Availability; Black People; Body Weight; D	2007
DPP-4 inhibitors. Best practice & research. Clinical endocrinology & metabolism, 2007, Volume: 21, Issue:4 Topics: Adamantane; Animals; Body Weight; Diabetes Mellitus, Type 2; Dipeptidyl-Peptidase IV Inhibitors; Dru	2007
Cardiovascular risk in women with polycystic ovary syndrome. Minerva endocrinologica, 2007, Volume: 32, Issue:4 Topics: Atherosclerosis; Biomarkers; Body Weight; Cardiovascular Diseases; Diabetes Mellitus, Type 2; Exerci	2007
Clinical trials with thiazolidinediones in subjects with Type 2 diabetes--is pioglitazone any different from rosiglitazone? Expert opinion on pharmacotherapy, 2008, Volume: 9, Issue:3 Topics: Biomarkers; Body Weight; Diabetes Mellitus, Type 2; Humans; Hypoglycemic Agents; Insulin Resistance;	2008