Compounds > primaquine
Page last updated: 2024-11-03

primaquine and Parasitemia

primaquine has been researched along with Parasitemia in 80 studies

Primaquine: An aminoquinoline that is given by mouth to produce a radical cure and prevent relapse of vivax and ovale malarias following treatment with a blood schizontocide. It has also been used to prevent transmission of falciparum malaria by those returning to areas where there is a potential for re-introduction of malaria. Adverse effects include anemias and GI disturbances. (From Martindale, The Extra Pharmacopeia, 30th ed, p404)
primaquine : An N-substituted diamine that is pentane-1,4-diamine substituted by a 6-methoxyquinolin-8-yl group at the N(4) position. It is a drug used in the treatment of malaria and Pneumocystis pneumonia.

Parasitemia: The presence of parasites (especially malarial parasites) in the blood. (Dorland, 27th ed)

Research Excerpts

ExcerptRelevanceReference
"5 days) high-dose (1 mg/kg twice daily) primaquine (PQ) for uncomplicated malaria because of any Plasmodium species in children randomized to early- or delayed treatment."9.69Ultra-short course, high-dose primaquine to prevent Plasmodium vivax infection following uncomplicated pediatric malaria: A randomized, open-label, non-inferiority trial of early versus delayed treatment. ( Batty, KT; Davis, TME; Kasian, B; Laman, M; Lorry, L; Manning, L; Moore, BR; Pomat, W; Robinson, LJ; Salman, S; Tesine, P; Woon, SA; Yadi, G; Yambo, P, 2023)
"Tafenoquine, a single-dose therapy for Plasmodium vivax malaria, has been associated with relapse prevention through the clearance of P."9.30Tafenoquine versus Primaquine to Prevent Relapse of Plasmodium vivax Malaria. ( Angus, B; Aruachan, S; Bancone, G; Breton, JJ; Brito, MAM; Casapía, M; Chu, CS; Chuquiyauri, R; Clover, DD; Costa, MRF; Craig, G; Duparc, S; Green, JA; Hardaker, E; Hien, TT; Jones, SW; Kendall, L; Koh, GCKW; Lacerda, MVG; Llanos-Cuentas, A; Mohamed, K; Monteiro, WM; Namaik-Larp, C; Nguyen, CH; Nosten, FH; Papwijitsil, R; Rousell, VM; Val, F; Vélez, ID; Villegas, MF; Wilches, VM, 2019)
"Primaquine is the only widely used drug that prevents Plasmodium vivax malaria relapses, but adherence to the standard 14-day regimen is poor."9.30Short-course primaquine for the radical cure of Plasmodium vivax malaria: a multicentre, randomised, placebo-controlled non-inferiority trial. ( Assawariyathipat, T; Assefa, A; Auburn, S; Baird, JK; Chand, K; Chau, NH; Cheah, PY; Day, NP; Degaga, TS; Devine, A; Dhorda, M; Dondorp, A; Dong, LT; Ekawati, LL; Fahmi, F; Hailu, A; Hasanzai, MA; Hien, TT; Khu, H; Ley, B; Lubell, Y; Marfurt, J; Mohammad, H; Moore, KA; Naddim, MN; Pasaribu, AP; Pasaribu, S; Price, RN; Promnarate, C; Rahim, AG; Simpson, JA; Sirithiranont, P; Solomon, H; Sudoyo, H; Sutanto, I; Taylor, WRJ; Thanh, NV; Thriemer, K; Tuyet-Trinh, NT; von Seidlein, L; Waithira, N; White, NJ; Woyessa, A; Yamin, FY; Yuentrakul, P, 2019)
" Artesunate cleared parasitemia significantly faster than chloroquine."9.27Comparison of the Cumulative Efficacy and Safety of Chloroquine, Artesunate, and Chloroquine-Primaquine in Plasmodium vivax Malaria. ( Aung, AA; Bancone, G; Carrara, VI; Cheah, PY; Chu, CS; Chue, AL; Imwong, M; Lwin, KM; Moore, KA; Nosten, F; Phyo, AP; Proux, S; Raksapraidee, R; San, T; Sriprawat, K; Tarning, J; Watson, J; White, NJ; Wiladphaingern, J; Win, HH; Winterberg, M, 2018)
"Adults with Plasmodium falciparum malaria were randomized to receive 1 of 3 artemisinin combination therapies (ACTs) with or without primaquine (0."9.24Safety and Efficacy of Adding a Single Low Dose of Primaquine to the Treatment of Adult Patients With Plasmodium falciparum Malaria in Senegal, to Reduce Gametocyte Carriage: A Randomized Controlled Trial. ( Fall, FB; Faye, B; Faye, BT; Gaye, O; Greenwood, B; Milligan, P; Ndiaye, JL; Ndiaye, M; Poirot, E; Sow, D; Sylla, K; Tine, RC; Wang, D, 2017)
"The efficacy of a single dose of 45 mg primaquine, as a gametocytocidal agent, was assessed in Mumbai, India, among adults with uncomplicated or severe Plasmodium falciparum malaria."9.11A prospective study evaluating the efficacy of a single, 45-mg dose of primaquine, as a gametocytocidal agent, in patients with Plasmodium falciparum malaria in Mumbai, India. ( Aigal, U; Chogle, AR; Dalvi, SS; Gogtay, NJ; Kamtekar, KD; Karnad, DR; Kshirsagar, NA, 2004)
", Basel Switzerland) (pyrimethamine and sulfadoxine), primaquine in a high dose, and artesunate for treating acute Plasmodium vivax malaria, we conducted a comparative clinical trial of these 3 drugs in an open-label study."9.09Efficacy of primaquine regimens for primaquine-resistant Plasmodium vivax malaria in Thailand. ( Bussaratid, V; Krudsood, S; Looareesuwan, S; Phumratanaprapin, W; Silachamroon, U; Singhasivanon, P; Srivilirit, S; Treeprasertsuk, S; Wilairatana, P, 1999)
"Primaquine (PQ) is one of the most widely used antimalarial and is the only available drug till date to combat relapsing form of malaria especially in case of Plasmodium vivax and Plasmodium ovale."7.74Formulation, antimalarial activity and biodistribution of oral lipid nanoemulsion of primaquine. ( Singh, KK; Vingkar, SK, 2008)
"The aim of this preliminary study was to investigate the potential use of the transdermal route for primaquine administration in the treatment of malaria."7.69Preliminary evaluation of primaquine activity on rodent malaria model after transdermal administration. ( Couarraze, G; Deharo, E; Landau, I; Mayorga, P, 1997)
" Blood samples were collected for parasite detection (by microscopy and PCR), molecular genotyping and pharmacokinetic analyses."6.94Parasite clearance, cure rate, post-treatment prophylaxis and safety of standard 3-day versus an extended 6-day treatment of artemether-lumefantrine and a single low-dose primaquine for uncomplicated Plasmodium falciparum malaria in Bagamoyo district, Tan ( Barnes, R; Björkman, A; Kitabi, EN; Mårtensson, A; Mhamilawa, LE; Mmbando, BP; Morris, U; Ngasala, B; Soe, AP, 2020)
"Tafenoquine is a single-dose 8-aminoquinoline that has recently been registered for the radical cure of P."6.90Single-Dose Tafenoquine to Prevent Relapse of Plasmodium vivax Malaria. ( Abdissa, A; Abebe, C; Angus, B; Batista Pereira, D; Beck, HP; Brand, F; Breton, JJ; Brito, MAM; Buathong, N; Casapía, M; Chuquiyauri, R; Clover, DD; Costa, MRF; Diro, E; Duparc, S; Espino, FEJ; Fletcher, K; Getie, S; Green, JA; Hardaker, E; Jones, SW; Kellam, LM; Kleim, JP; Koh, GCKW; Krudsood, S; Lacerda, MVG; Llanos-Cuentas, A; Lon, C; Mia, RZ; Mohamed, K; Mohammed, R; Monteiro, WM; Noedl, H; Rousell, VM; Saunders, DL; Tada, MS; Ugwuegbulam, CO; Val, F; Wubie, KM; Yilma, D; Zeynudin, A, 2019)
"Plasmodium vivax malaria is an important cause of morbidity in Central and South America."6.72Efficacy of three chloroquine-primaquine regimens for treatment of Plasmodium vivax malaria in Colombia. ( Alvarez, G; Blair, S; Carmona-Fonseca, J; Maestre, A; Piñeros, JG; Ríos, A; Tobón, A, 2006)
"TQ 300 mg single dose reduces P vivax recurrences compared to no antihypnozoite treatment during a six-month follow-up, but there is moderate uncertainty around effect size (RR 0."6.66Tafenoquine for preventing relapse in people with Plasmodium vivax malaria. ( Fernando, D; Rajapakse, S; Rodrigo, C, 2020)
"5 days) high-dose (1 mg/kg twice daily) primaquine (PQ) for uncomplicated malaria because of any Plasmodium species in children randomized to early- or delayed treatment."5.69Ultra-short course, high-dose primaquine to prevent Plasmodium vivax infection following uncomplicated pediatric malaria: A randomized, open-label, non-inferiority trial of early versus delayed treatment. ( Batty, KT; Davis, TME; Kasian, B; Laman, M; Lorry, L; Manning, L; Moore, BR; Pomat, W; Robinson, LJ; Salman, S; Tesine, P; Woon, SA; Yadi, G; Yambo, P, 2023)
"Tafenoquine, a single-dose therapy for Plasmodium vivax malaria, has been associated with relapse prevention through the clearance of P."5.30Tafenoquine versus Primaquine to Prevent Relapse of Plasmodium vivax Malaria. ( Angus, B; Aruachan, S; Bancone, G; Breton, JJ; Brito, MAM; Casapía, M; Chu, CS; Chuquiyauri, R; Clover, DD; Costa, MRF; Craig, G; Duparc, S; Green, JA; Hardaker, E; Hien, TT; Jones, SW; Kendall, L; Koh, GCKW; Lacerda, MVG; Llanos-Cuentas, A; Mohamed, K; Monteiro, WM; Namaik-Larp, C; Nguyen, CH; Nosten, FH; Papwijitsil, R; Rousell, VM; Val, F; Vélez, ID; Villegas, MF; Wilches, VM, 2019)
"Primaquine is the only widely used drug that prevents Plasmodium vivax malaria relapses, but adherence to the standard 14-day regimen is poor."5.30Short-course primaquine for the radical cure of Plasmodium vivax malaria: a multicentre, randomised, placebo-controlled non-inferiority trial. ( Assawariyathipat, T; Assefa, A; Auburn, S; Baird, JK; Chand, K; Chau, NH; Cheah, PY; Day, NP; Degaga, TS; Devine, A; Dhorda, M; Dondorp, A; Dong, LT; Ekawati, LL; Fahmi, F; Hailu, A; Hasanzai, MA; Hien, TT; Khu, H; Ley, B; Lubell, Y; Marfurt, J; Mohammad, H; Moore, KA; Naddim, MN; Pasaribu, AP; Pasaribu, S; Price, RN; Promnarate, C; Rahim, AG; Simpson, JA; Sirithiranont, P; Solomon, H; Sudoyo, H; Sutanto, I; Taylor, WRJ; Thanh, NV; Thriemer, K; Tuyet-Trinh, NT; von Seidlein, L; Waithira, N; White, NJ; Woyessa, A; Yamin, FY; Yuentrakul, P, 2019)
" This result suggests that the transdermal route may be a very interesting approach for malaria prophylaxis and should encourage further studies in order to determine the absolute bioavailability of the drug as well as its dose-effect relationship."5.30Rodent malaria prophylaxis by transdermal delivery of primaquine. ( Coquelin, F; Couarraze, G; Mayorga, P; Miltgen, F, 1998)
" Artesunate cleared parasitemia significantly faster than chloroquine."5.27Comparison of the Cumulative Efficacy and Safety of Chloroquine, Artesunate, and Chloroquine-Primaquine in Plasmodium vivax Malaria. ( Aung, AA; Bancone, G; Carrara, VI; Cheah, PY; Chu, CS; Chue, AL; Imwong, M; Lwin, KM; Moore, KA; Nosten, F; Phyo, AP; Proux, S; Raksapraidee, R; San, T; Sriprawat, K; Tarning, J; Watson, J; White, NJ; Wiladphaingern, J; Win, HH; Winterberg, M, 2018)
"Adults with Plasmodium falciparum malaria were randomized to receive 1 of 3 artemisinin combination therapies (ACTs) with or without primaquine (0."5.24Safety and Efficacy of Adding a Single Low Dose of Primaquine to the Treatment of Adult Patients With Plasmodium falciparum Malaria in Senegal, to Reduce Gametocyte Carriage: A Randomized Controlled Trial. ( Fall, FB; Faye, B; Faye, BT; Gaye, O; Greenwood, B; Milligan, P; Ndiaye, JL; Ndiaye, M; Poirot, E; Sow, D; Sylla, K; Tine, RC; Wang, D, 2017)
"Chloroquine plus primaqine is an inexpensive and highly effective treatment for uncomplicated knowlesi malaria infections in humans and there is no evidence of drug resistance."5.14Clinical and parasitological response to oral chloroquine and primaquine in uncomplicated human Plasmodium knowlesi infections. ( Cox-Singh, J; Daneshvar, C; Davis, TM; Divis, PC; Rafa'ee, MZ; Singh, B; Zakaria, SK, 2010)
"The efficacy of a single dose of 45 mg primaquine, as a gametocytocidal agent, was assessed in Mumbai, India, among adults with uncomplicated or severe Plasmodium falciparum malaria."5.11A prospective study evaluating the efficacy of a single, 45-mg dose of primaquine, as a gametocytocidal agent, in patients with Plasmodium falciparum malaria in Mumbai, India. ( Aigal, U; Chogle, AR; Dalvi, SS; Gogtay, NJ; Kamtekar, KD; Karnad, DR; Kshirsagar, NA, 2004)
"An open randomized controlled study of mefloquine-artesunate and mefloquine-primaquine for the treatment of uncomplicated Plasmodium falciparum malaria was carried out in Kanchanaburi in the Saiyok District in western Thailand."5.10The efficacy of combined mefloquine-artesunate versus mefloquine-primaquine on subsequent development of Plasmodium falciparum gametocytemia. ( Chaikachonpatd, S; Chanthapakajee, K; Chindarat, S; Kaewkaukul, N; Lim, K; Silpasakorn, S; Suputtamongkol, Y; Thamlikitkul, V, 2003)
", Basel Switzerland) (pyrimethamine and sulfadoxine), primaquine in a high dose, and artesunate for treating acute Plasmodium vivax malaria, we conducted a comparative clinical trial of these 3 drugs in an open-label study."5.09Efficacy of primaquine regimens for primaquine-resistant Plasmodium vivax malaria in Thailand. ( Bussaratid, V; Krudsood, S; Looareesuwan, S; Phumratanaprapin, W; Silachamroon, U; Singhasivanon, P; Srivilirit, S; Treeprasertsuk, S; Wilairatana, P, 1999)
"Ethiopia rolled out primaquine nationwide in 2018 for radical cure along with chloroquine for the treatment of uncomplicated Plasmodium vivax malaria in its bid for malaria elimination by 2030."4.31Treatment of uncomplicated Plasmodium vivax with chloroquine plus radical cure with primaquine without G6PDd testing is safe in Arba Minch, Ethiopia: assessment of clinical and parasitological response. ( Abadura, GS; Bayissa, GA; Behaksra, SW; Bulto, MG; Gadisa, E; Mekonnen, DA; Tadesse, FG; Taffese, HS; Tessema, TS, 2023)
"Primaquine (PQ) is one of the most widely used antimalarial drugs and is the only available drug that combats the relapsing form of malaria."3.80Preparation, characterization, and optimization of primaquine-loaded solid lipid nanoparticles. ( Gathirwa, JW; Kalombo, L; Mahanga, GM; Melariri, P; Ogutu, B; Oloo, F; Omwoyo, WN; Swai, H, 2014)
" After sporozoite inoculation and blood-stage cure of initial parasitemia with chloroquine, rhesus macaques were treated on subsequent relapses with chloroquine in conjunction with test regimens of approved drugs."3.78Use of a rhesus Plasmodium cynomolgi model to screen for anti-hypnozoite activity of pharmaceutical substances. ( Bennett, K; Deye, GA; Fracisco, S; Gettayacamin, M; Hansukjariya, P; Im-erbsin, R; Macareo, L; Magill, AJ; Ohrt, C; Rothstein, Y; Sattabongkot, J, 2012)
" Sexual and asexual parasite dynamics were thus evaluated in patients involved in antimalarial drug efficacy studies by using combined treatment with and without artemisinin derivatives for treating uncomplicated acute Plasmodium falciparum malaria in Antioquia, Colombia."3.76Dynamics of Plasmodium falciparum parasitemia regarding combined treatment regimens for acute uncomplicated malaria, Antioquia, Colombia. ( Alvarez, G; Blair, S; Piñeros, JG; Ríos, A; Tobón, A, 2010)
" knowlesi infection had uncomplicated malaria that responded to chloroquine and primaquine treatment."3.75Clinical and laboratory features of human Plasmodium knowlesi infection. ( Cox-Singh, J; Daneshvar, C; Davis, TM; Divis, PC; Rafa'ee, MZ; Singh, B; Zakaria, SK, 2009)
"Primaquine (PQ) is one of the most widely used antimalarial and is the only available drug till date to combat relapsing form of malaria especially in case of Plasmodium vivax and Plasmodium ovale."3.74Formulation, antimalarial activity and biodistribution of oral lipid nanoemulsion of primaquine. ( Singh, KK; Vingkar, SK, 2008)
"A new 8-aminoquinoline antimalarial WR 238605 (Tafenoquine), developed initially as a primaquine alternative for prevention of Plasmodium vivax relapses was evaluated for blood schizontocidal activity against two simian malaria infections namely Plasmodium cynomolgi B and Plasmodium fragile in rhesus monkeys."3.72Blood schizontocidal activity of WR 238605 (Tafenoquine) against Plasmodium cynomolgi and Plasmodium fragile infections in rhesus monkeys. ( Dutta, GP; Puri, SK, 2003)
"The spectrum of antimalarial activity of the new macrolide antibiotic azithromycin was evaluated against blood- and sporozoite-induced infections with a chloroquine-resistant strain of Plasmodium yoelii nigeriensis (N-67) in Swiss mice and with simian parasite Plasmodium cynomolgi B in rhesus monkeys."3.70Azithromycin: antimalarial profile against blood- and sporozoite-induced infections in mice and monkeys. ( Puri, SK; Singh, N, 2000)
"The aim of this preliminary study was to investigate the potential use of the transdermal route for primaquine administration in the treatment of malaria."3.69Preliminary evaluation of primaquine activity on rodent malaria model after transdermal administration. ( Couarraze, G; Deharo, E; Landau, I; Mayorga, P, 1997)
" Blood samples were collected for parasite detection (by microscopy and PCR), molecular genotyping and pharmacokinetic analyses."2.94Parasite clearance, cure rate, post-treatment prophylaxis and safety of standard 3-day versus an extended 6-day treatment of artemether-lumefantrine and a single low-dose primaquine for uncomplicated Plasmodium falciparum malaria in Bagamoyo district, Tan ( Barnes, R; Björkman, A; Kitabi, EN; Mårtensson, A; Mhamilawa, LE; Mmbando, BP; Morris, U; Ngasala, B; Soe, AP, 2020)
"Tafenoquine is a single-dose 8-aminoquinoline that has recently been registered for the radical cure of P."2.90Single-Dose Tafenoquine to Prevent Relapse of Plasmodium vivax Malaria. ( Abdissa, A; Abebe, C; Angus, B; Batista Pereira, D; Beck, HP; Brand, F; Breton, JJ; Brito, MAM; Buathong, N; Casapía, M; Chuquiyauri, R; Clover, DD; Costa, MRF; Diro, E; Duparc, S; Espino, FEJ; Fletcher, K; Getie, S; Green, JA; Hardaker, E; Jones, SW; Kellam, LM; Kleim, JP; Koh, GCKW; Krudsood, S; Lacerda, MVG; Llanos-Cuentas, A; Lon, C; Mia, RZ; Mohamed, K; Mohammed, R; Monteiro, WM; Noedl, H; Rousell, VM; Saunders, DL; Tada, MS; Ugwuegbulam, CO; Val, F; Wubie, KM; Yilma, D; Zeynudin, A, 2019)
"Primaquine was well tolerated and could be administered along with an artemisinin combination therapy as the first-line therapy."2.78Nonrandomized controlled trial of artesunate plus sulfadoxine-pyrimethamine with or without primaquine for preventing posttreatment circulation of Plasmodium falciparum gametocytes. ( Anvikar, A; Juliano, JJ; MacDonald, PD; Meshnick, SR; Mishra, N; Poole, C; Schapira, A; Shah, NK; Srivastava, B; Valecha, N, 2013)
"A safe and reproducible Plasmodium vivax infectious challenge method is required to evaluate the efficacy of malaria vaccine candidates."2.76Consistent safety and infectivity in sporozoite challenge model of Plasmodium vivax in malaria-naive human volunteers. ( Arévalo-Herrera, M; Echavarría, JF; Epstein, JE; Herrera, S; Jordán-Villegas, A; Palacios, R; Ramírez, O; Richie, TL; Rocha, L; Solarte, Y; Vélez, JD, 2011)
" The impact of MDA with the gametocytocidal drug combination sulphadoxine-pyrimethamine (SP) plus artesunate (AS) plus primaquine (PQ, single dose 0."2.76A cluster-randomized trial of mass drug administration with a gametocytocidal drug combination to interrupt malaria transmission in a low endemic area in Tanzania. ( Bousema, T; Drakeley, C; Gosling, R; Hermsen, R; Masokoto, A; Mosha, F; Mwanziva, C; Okell, L; Sauerwein, R; Semvua, S; Shekalaghe, SA; Teelen, K; ter Braak, R; van den Bijllaardt, W; van den Bosch, S, 2011)
"Plasmodium vivax malaria is an important cause of morbidity in Central and South America."2.72Efficacy of three chloroquine-primaquine regimens for treatment of Plasmodium vivax malaria in Colombia. ( Alvarez, G; Blair, S; Carmona-Fonseca, J; Maestre, A; Piñeros, JG; Ríos, A; Tobón, A, 2006)
"Chloroquine combined with primaquine was evaluated for therapy of uncomplicated malaria caused by Plasmodium falciparum in nonimmune Javanese migrants to northeastern Papua, Indonesia."2.70Short report: therapeutic efficacy of chloroquine combined with primaquine against Plasmodium falciparum in northeastern Papua, Indonesia. ( Ayomi, E; Baird, JK; Basri, H; Fryauff, DJ; Hoffman, SL; Sutanihardja, A; Wiady, I, 2002)
"Primaquine was better tolerated than chloroquine."2.68Primaquine for prophylaxis against malaria among nonimmune transmigrants in Irian Jaya, Indonesia. ( Baird, JK; Bangs, MJ; Basri, H; Fryauff, DJ; Leksana, B; Masbar, S; Richie, TL; Subianto, B; Wiady, I, 1995)
"Halofantrine-primaquine was significantly more effective than chloroquine-primaquine against falciparum malaria (P < 0."2.68Halofantrine and primaquine for radical cure of malaria in Irian Jaya, Indonesia. ( Baird, JK; Bangs, MJ; Basri, H; Fryauff, DJ; Harjosuwarno, S; Hoffman, SL; Richie, TL; Subianto, B; Tjitra, E; Wiady, I, 1997)
"TQ 300 mg single dose reduces P vivax recurrences compared to no antihypnozoite treatment during a six-month follow-up, but there is moderate uncertainty around effect size (RR 0."2.66Tafenoquine for preventing relapse in people with Plasmodium vivax malaria. ( Fernando, D; Rajapakse, S; Rodrigo, C, 2020)
"Malaria recurrences after an initially successful therapy and malarial fever occurring a long time after infection are well-known problems in malariology."2.53Clinical implications of a gradual dormancy concept in malaria. ( Franken, G; Holtfreter, MC; Labisch, A; Mehlhorn, H; Richter, J; Walter, S, 2016)
"Here we describe high rates of P."1.35Recurrent parasitemias and population dynamics of Plasmodium vivax polymorphisms in rural Amazonia. ( da Silva, NS; da Silva-Nunes, M; Ferreira, MU; Orjuela-Sánchez, P, 2009)
" This result suggests that the transdermal route may be a very interesting approach for malaria prophylaxis and should encourage further studies in order to determine the absolute bioavailability of the drug as well as its dose-effect relationship."1.30Rodent malaria prophylaxis by transdermal delivery of primaquine. ( Coquelin, F; Couarraze, G; Mayorga, P; Miltgen, F, 1998)

Research

Studies (80)

TimeframeStudies, this research(%)All Research%
pre-19901 (1.25)18.7374
1990's10 (12.50)18.2507
2000's23 (28.75)29.6817
2010's39 (48.75)24.3611
2020's7 (8.75)2.80

Authors

AuthorsStudies
Cohen, A1
Suzanne, P1
Lancelot, JC1
Verhaeghe, P1
Lesnard, A1
Basmaciyan, L1
Hutter, S1
Laget, M1
Dumètre, A1
Paloque, L1
Deharo, E3
Crozet, MD1
Rathelot, P1
Dallemagne, P1
Lorthiois, A1
Sibley, CH1
Vanelle, P1
Valentin, A2
Mazier, D1
Rault, S1
Azas, N1
Quiliano, M1
Pabón, A1
Moles, E1
Bonilla-Ramirez, L1
Fabing, I1
Fong, KY1
Nieto-Aco, DA1
Wright, DW1
Pizarro, JC1
Vettorazzi, A1
López de Cerain, A1
Fernández-Busquets, X2
Garavito, G1
Aldana, I1
Galiano, S1
Morais, CMG1
Brito, RMM1
Weselucha-Birczyńska, A1
Pereira, VSS1
Pereira-Silva, JW1
Menezes, A1
Pessoa, FAC1
Kucharska, M1
Birczyńska-Zych, M1
Ríos-Velásquez, CM1
de Andrade-Neto, VF1
Woon, SA1
Moore, BR1
Laman, M1
Tesine, P1
Lorry, L1
Kasian, B1
Yambo, P1
Yadi, G1
Pomat, W1
Batty, KT1
Salman, S1
Robinson, LJ1
Davis, TME1
Manning, L1
Mekonnen, DA1
Abadura, GS1
Behaksra, SW1
Taffese, HS1
Bayissa, GA1
Bulto, MG1
Tessema, TS1
Tadesse, FG1
Gadisa, E1
Thriemer, K2
Degaga, TS2
Christian, M1
Alam, MS1
Rajasekhar, M1
Ley, B2
Hossain, MS1
Kibria, MG1
Tego, TT1
Abate, DT1
Weston, S1
Mnjala, H1
Rumaseb, A1
Satyagraha, AW1
Sadhewa, A1
Panggalo, LV1
Ekawati, LL2
Lee, G1
Anose, RT1
Kiros, FG1
Simpson, JA2
Karahalios, A1
Woyessa, A2
Baird, JK6
Sutanto, I2
Hailu, A2
Price, RN2
Chughlay, MF1
Akakpo, S1
Odedra, A1
Csermak-Renner, K1
Djeriou, E1
Winnips, C1
Leboulleux, D1
Gaur, AH1
Shanks, GD1
McCarthy, J1
Chalon, S1
Mhamilawa, LE1
Ngasala, B2
Morris, U1
Kitabi, EN1
Barnes, R1
Soe, AP1
Mmbando, BP1
Björkman, A2
Mårtensson, A2
Rodrigo, C1
Rajapakse, S1
Fernando, D1
Gunawardena, S1
Daniels, RF1
Yahathugoda, TC1
Weerasooriya, MV1
Durfee, K1
Volkman, SK1
Wirth, DF1
Karunaweera, ND1
Tine, RC1
Sylla, K1
Faye, BT1
Poirot, E1
Fall, FB1
Sow, D1
Wang, D1
Ndiaye, M1
Ndiaye, JL1
Faye, B1
Greenwood, B1
Gaye, O1
Milligan, P1
Sortica, VA1
Lindenau, JD1
Cunha, MG1
O Ohnishi, MD1
R Ventura, AM1
Ribeiro-Dos-Santos, ÂK1
Santos, SE1
Guimarães, LS1
Hutz, MH1
Deng, C2
Huang, B1
Wang, Q1
Wu, W1
Zheng, S1
Zhang, H1
Li, D1
Feng, D1
Li, G2
Xue, L1
Yang, T1
Tuo, F1
Mohadji, F1
Su, XZ1
Xu, Q1
Wu, Z1
Lin, L1
Zhou, J1
Yan, H1
Bacar, A1
Said Abdallah, K1
Kéké, RA1
Msa Mliva, A1
Mohamed, M1
Wang, X1
Huang, S1
Oithik, F1
Li, XB1
Lu, F1
Fay, MP1
Liu, XH1
Wellems, TE1
Song, J2
Chu, CS2
Phyo, AP1
Lwin, KM1
Win, HH1
San, T1
Aung, AA1
Raksapraidee, R1
Carrara, VI1
Bancone, G2
Watson, J1
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Wiladphaingern, J1
Proux, S1
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Winterberg, M1
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Chue, AL1
Tarning, J1
Imwong, M1
Nosten, F1
White, NJ3
Lacerda, MVG2
Llanos-Cuentas, A2
Krudsood, S4
Lon, C1
Saunders, DL1
Mohammed, R1
Yilma, D1
Batista Pereira, D1
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Chuquiyauri, R2
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Casapía, M2
Monteiro, WM2
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Costa, MRF2
Buathong, N1
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Ugwuegbulam, CO1
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Papwijitsil, R1
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Dysoley, L1
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von Seidlein, L1
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Demeke, L1
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Nettey, H1
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Kachur, SP1
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Rénia, L1
Lacerda, MV2
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Sohsuebngarm, D1
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Nithiuthai, S1
Chansiripornchai, N1
Laothamatas, J1
Sammet, CL1
Golay, X1
Van Cauteren, M1
Lekprasert, V1
Tangpukdee, N2
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Swaminathan, SV1
DeLaPaz, RL1
Brown, TR1
Looareesuwan, S4
Brittenham, GM1
Oki, M1
Asai, S1
Saito-Nakano, Y1
Nakayama, T1
Tanaka, Y1
Tachibana, H1
Ohmae, H1
Nozaki, T1
Miyachi, H1
DiTusa, C1
Kozar, MP1
Pybus, B1
Sousa, J1
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Gettayacamin, M2
Im-erbsin, R2
Tungtaeng, A1
Ohrt, C2
Dos-Santos, JC1
Angerami, RN1
Castiñeiras, CM1
Garcia, MT1
Levy, CE1
Moretti, ML1
Omwoyo, WN1
Ogutu, B1
Oloo, F1
Swai, H1
Kalombo, L1
Melariri, P1
Mahanga, GM1
Gathirwa, JW1
Raccurt, CP1
Brasseur, P1
Lemoine, F1
Cicéron, M1
Existe, A1
Boncy, J1
Richter, J1
Franken, G1
Holtfreter, MC1
Walter, S1
Labisch, A1
Mehlhorn, H1
Mwaiswelo, R1
Jovel, I1
Aydin-Schmidt, B1
Gosling, R2
Premji, Z1
Mmbando, B1
Lawpoolsri, S1
Klein, EY1
Singhasivanon, P2
Yimsamran, S1
Thanyavanich, N1
Maneeboonyang, W1
Hungerford, LL1
Maguire, JH1
Smith, DL1
Daneshvar, C2
Davis, TM2
Cox-Singh, J2
Rafa'ee, MZ2
Zakaria, SK2
Divis, PC2
Singh, B2
Yeshiwondim, AK1
Tekle, AH1
Dengela, DO1
Yohannes, AM1
Teklehaimanot, A1
Orjuela-Sánchez, P1
da Silva, NS1
da Silva-Nunes, M1
Ferreira, MU1
Vásquez, AM1
Sanín, F1
Alvarez, LG1
Tobón, A3
Ríos, A3
Blair, S3
Chevalley, S1
Coste, A1
Lopez, A1
Pipy, B1
Socheat, D1
Tan, B1
Dara, P1
Sokunthea, S1
Seila, S1
Ou, F1
Jian, H1
Bousema, T2
Okell, L2
Shekalaghe, S1
Griffin, JT1
Omar, S1
Sawa, P1
Sutherland, C1
Sauerwein, R2
Ghani, AC1
Drakeley, C2
Alvarez, G2
Piñeros, JG2
Herrera, S1
Solarte, Y1
Jordán-Villegas, A1
Echavarría, JF1
Rocha, L1
Palacios, R1
Ramírez, O1
Vélez, JD1
Epstein, JE1
Richie, TL4
Arévalo-Herrera, M1
Capela, R1
Cabal, GG1
Rosenthal, PJ1
Gut, J1
Mota, MM1
Moreira, R1
Lopes, F1
Prudêncio, M1
Shekalaghe, SA1
van den Bosch, S1
ter Braak, R1
van den Bijllaardt, W1
Mwanziva, C1
Semvua, S1
Masokoto, A1
Mosha, F1
Teelen, K1
Hermsen, R1
Arango, EM1
Upegui, YA1
Carmona-Fonseca, J2
Congpuon, K1
Satimai, W2
Sujariyakul, A1
Intanakom, S1
Harnpitakpong, W1
Pranuth, Y1
Cholpol, S1
Bualombai, P1
Deye, GA1
Hansukjariya, P1
Sattabongkot, J1
Rothstein, Y1
Macareo, L1
Fracisco, S1
Bennett, K1
Magill, AJ1
Qiao, LG1
Qi, G1
Luzzatto, L1
Wiady, I3
Sutanihardja, A1
Basri, H3
Ayomi, E1
Fryauff, DJ4
Hoffman, SL3
Puri, SK2
Dutta, GP1
Suputtamongkol, Y1
Chindarat, S1
Silpasakorn, S1
Chaikachonpatd, S1
Lim, K1
Chanthapakajee, K1
Kaewkaukul, N1
Thamlikitkul, V1
Machado, RL1
de Figuereido Filho, AF1
Calvosa, VS1
Figueredo, MC1
Nascimento, JM1
Póvoa, MM1
Giao, PT1
de Vries, PJ1
Hung, le Q1
Binh, TQ1
Nam, NV1
Kager, PA1
Kamtekar, KD3
Gogtay, NJ3
Dalvi, SS3
Karnad, DR1
Chogle, AR3
Aigal, U3
Kshirsagar, NA3
Vijaykadga, S1
Rojanawatsirivej, C1
Congpoung, K1
Uaekowitchai, C1
Pumborplub, B1
Sittimongkol, S1
Pinyorattanachote, A1
Prigchoo, P1
Spudick, JM1
Garcia, LS1
Graham, DM1
Haake, DA1
Dunne, MW1
Singh, N2
Shukla, M1
Bhattacharyya, PC1
Patel, K1
Mohapatra, MK1
Lakhani, J1
Devi, CU1
Adak, T1
Dev, V1
Yadav, RS1
Lele, C1
Patki, K1
Mehta, SS1
Maestre, A1
Murphy, SC1
Fernandez-Pol, S1
Chung, PH1
Prasanna Murthy, SN1
Milne, SB1
Salomao, M1
Brown, HA1
Lomasney, JW1
Mohandas, N1
Haldar, K1
Muangnoicharoen, S1
Thanachartwet, V1
Luplertlop, N1
Srivilairit, S1
Kano, S1
Ringwald, P1
Singh, KK1
Vingkar, SK1
Bangs, MJ2
Subianto, B3
Leksana, B1
Masbar, S1
Cranfield, MR1
Graczyk, TK1
Beall, FB1
Ialeggio, DM1
Shaw, ML1
Skjoldager, ML1
Awalludin, M1
Jones, T1
Tjitra, E2
Wignall, FS1
Harjosuwarno, S1
Mayorga, P2
Landau, I1
Couarraze, G2
Nayar, JK1
Baker, RH1
Knight, JW1
Sullivan, JS1
Morris, CL1
Richardson, BB1
Galland, GG1
Collins, WE1
Buchachart, K1
Chalermrut, K1
Rattanapong, Y1
Amradee, S1
Siripiphat, S1
Chullawichit, S1
Thimasan, K1
Ittiverakul, M1
Triampon, A1
Walsh, DS1
Miltgen, F1
Coquelin, F1
Menéndez Capote, RL1
López Chávez, AU1
Silachamroon, U1
Treeprasertsuk, S1
Bussaratid, V1
Phumratanaprapin, W1
Srivilirit, S1
Penzhorn, BL1
Lewis, BD1
López-Rebollar, LM1
Swan, GE1
Merino, S1
Moreno, J1
Sanz, JJ1
Arriero, E1
Soto, J1
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Jankowski, EA1

Clinical Trials (21)

Trial Overview

TrialPhaseEnrollmentStudy TypeStart DateStatus
"Aiming at Prolonging the Therapeutic Life Span of Artemisinin-based Combination Therapies (ACT) in an Era of Imminent Plasmodium Falciparum Resistance in Bagamoyo District, Tanzania - New Strategies With Old Tools"[NCT03241901]Phase 4280 participants (Actual)Interventional2017-07-27Completed
A Randomised Open Label Study Comparing the Efficacy of Chloroquine/Primaquine, Chloroquine and Artesunate in the Treatment of Vivax Malaria Along the Thai-Burmese Border[NCT01074905]Phase 3655 participants (Actual)Interventional2010-05-31Completed
Does Artemisinin Combination Treatment Reduce the Radical Curative Efficacy of High Dose Tafenoquine for Plasmodium Vivax Malaria?[NCT05788094]Phase 4388 participants (Anticipated)Interventional2023-06-26Recruiting
Safety, Tolerability and Pharmacokinetics of Tafenoquine After Weekly and Escalating Monthly Doses of Tafenoquine in Healthy Vietnamese Volunteers[NCT05203744]Phase 4200 participants (Anticipated)Interventional2022-05-10Not yet recruiting
A Multi-centre, Double-blind, Randomised, Parallel-group, Active Controlled Study to Evaluate the Efficacy, Safety and Tolerability of Tafenoquine (SB-252263, WR238605) in Subjects With Plasmodium Vivax Malaria.[NCT01376167]Phase 2851 participants (Actual)Interventional2014-04-24Completed
FocaL Mass Drug Administration for Vivax Malaria Elimination (FLAME): a Pragmatic Cluster Randomized Controlled Trial in Peru[NCT05690841]Phase 37,700 participants (Anticipated)Interventional2024-02-01Not yet recruiting
A Randomized, Double-Blind, Double Dummy, Comparative, Multicenter Study to Assess the Incidence of Hemolysis, Safety, and Efficacy of Tafenoquine (SB-252263, WR238605) Versus Primaquine in the Treatment of Subjects With Plasmodium Vivax Malaria[NCT02216123]Phase 3251 participants (Actual)Interventional2015-04-30Completed
The Tolerability and Safety of Low Dose Primaquine for Transmission Blocking in Symptomatic Falciparum Infected Cambodians[NCT02434952]Phase 4109 participants (Actual)Interventional2014-10-31Completed
Improving the Radical Cure of Vivax Malaria: A Multicentre Randomised Comparison of Short and Long Course Primaquine Regimens[NCT01814683]2,388 participants (Actual)Interventional2014-07-31Completed
Ethiopia In-vivo Efficacy Study 2009: Evaluating the Efficacy of Artemether-lumefantrine for the Treatment of Uncomplicated Plasmodium Falciparum Infection and Either Artemether-lumefantrine or Chloroquine for P. Vivax Infection[NCT01052584]354 participants (Actual)Interventional2009-10-31Completed
A Clinical Study to Assess the Safety and Feasibility of Controlled Blood-stage Plasmodium Vivax Human Malaria Infection Through Experimental Inoculation of Cryopreserved Infected Erythrocytes in Healthy Thai Adults[NCT05071079]16 participants (Anticipated)Interventional2022-05-23Recruiting
Phase 1/2a Open-label Dose Safety, Reactogenicity, Immunogenicity and Efficacy of the Candidate Plasmodium Vivax Malaria Protein 001 (VMP001) Administered Intramuscularly With GlaxoSmithKline (GSK) Biologicals' Adjuvant System AS01B in Healthy Malaria-Naï[NCT01157897]Phase 1/Phase 241 participants (Actual)Interventional2010-07-31Completed
Efficacy and Safety of a Single Low-dose Primaquine Added to Standard Artemether-lumefantrine Treatment for the Clearance of Plasmodium Falciparum Gametocytes.[NCT02090036]Phase 4220 participants (Actual)Interventional2014-07-31Completed
Evaluation of the Efficacy and Safety of Primaquine for Clearance of Gametocytes in Uncomplicated Falciparum Malaria in Uganda[NCT01365598]Phase 3468 participants (Actual)Interventional2011-12-31Completed
Comparison of the Susceptibility of Naive and Pre-immune Volunteers to Infectious Challenge With Viable Plasmodium Vivax Sporozoites.[NCT01585077]Phase 1/Phase 216 participants (Actual)Interventional2012-10-31Completed
Evaluation of the Protective Efficacy of a Vaccine Derived From the Synthetic CS Protein of Plasmodium Vivax[NCT02083068]Phase 232 participants (Actual)Interventional2014-08-31Completed
Impact of Mass Screening and Selective Treatment With Dihydroartemisinin-piperaquine Plus Primaquine on Malaria Transmission in High Endemic Area, Belu Regency, Nusa Tenggara Timur Province, Indonesia: a Randomized Cluster Trial[NCT01878357]Phase 41,488 participants (Actual)Interventional2013-06-30Completed
Mass-Drug Administration With a Gametocytocidal Drug Combination, a Model for a Transmission Blocking Vaccine[NCT00509015]6,000 participants (Anticipated)Interventional2008-02-29Completed
Targeted Chemo-elimination (TCE) to Eradicate Malaria in Areas of Suspected or Proven Artemisinin Resistance in Southeast Asia and South Asia[NCT01872702]8,000 participants (Actual)Interventional2013-04-30Completed
Efficacy of Chloroquine (CQ) Alone Compared to Concomitant CQ and Primaquine (PQ) for the Treatment of Uncomplicated Plasmodium Vivax Infection[NCT02691910]Phase 2/Phase 3204 participants (Actual)Interventional2014-08-31Completed
Evaluation of Reproducibility of a Sporozoite Challenge Model for Plasmodium Vivax in Human Volunteers[NCT00367380]Phase 218 participants (Actual)Interventional2006-12-31Completed
[information is prepared from clinicaltrials.gov, extracted Sep-2024]

Trial Outcomes

Number of Participants Who Received Blood Transfusion

The number of participants who received blood transfusion as a result of hemoglobin decline has been summarized. (NCT01376167)
Timeframe: Up to Day 180

InterventionParticipants (Number)
CQ Only0
TQ + CQ0
PQ + CQ0

Number of Participants With Acute Renal Failure

There were no participants with acute renal failure in the study. (NCT01376167)
Timeframe: Up to Day 180

InterventionParticipants (Number)
CQ Only0
TQ + CQ0
PQ + CQ0

Number of Participants With Recurrence-free Efficacy at 4 Months Post Dose

A participant (par) was considered to have demonstrated recurrence-free efficacy at 4 months if: a) Par had non-zero P vivax asexual parasite count at Baseline. b) Par showed initial clearance of P vivax parasitemia. c) Par had no positive asexual P vivax parasite count at any assessment prior to or on Study Day 130 following initial parasite clearance. d) Par did not take a concomitant medication with anti-malarial activity at any point between Study Day 1 and their last parasite assessment after Study Day 109 (up to and including Study Day 130). e) Par is parasite-free at 4 months defined as a negative asexual P vivax parasite count at the first parasite assessment performed after Study Day 109 (up to and including Study Day 130). Par were censored if they did not have P.vivax at Baseline, or took a drug with anti-malarial action despite not having malaria parasites or did not have a 4 month assessment. The number of par with recurrence-free efficacy at 4 months has been summarized. (NCT01376167)
Timeframe: 4 months post dose

InterventionParticipants (Number)
CQ Only47
TQ + CQ177
PQ + CQ90

Number of Participants With Recurrence-free Efficacy at 6 Months Post Dose

A participant was considered to have demonstrated recurrence-free efficacy at 6 months if: a) Participant had non-zero P vivax asexual parasite count at Baseline. b) Participant showed initial clearance of P vivax parasitemia defined as two negative asexual P vivax parasite counts, with at least 6 hours between the counts, and no positive counts in the interval. c) Participant had no positive asexual P vivax parasite count at any assessment prior to or on Study Day 201 following initial parasite clearance. d) Participant did not take a concomitant medication with anti-malarial activity at any point between Study Day 1 and their last parasite assessment. e) Participant is parasite-free at 6 months. Participants were censored if they did not have P.vivax at Baseline, or took a drug with anti-malarial action despite not having malaria parasites, or did not have a 6 month assessment. The number of participants with recurrence-free efficacy at 6 months has been summarized. (NCT01376167)
Timeframe: 6 months post dose

InterventionParticipants (Number)
CQ Only35
TQ + CQ155
PQ + CQ83

Oral Clearance (CL/F) of TQ

Apparent population oral clearance of TQ (NCT01376167)
Timeframe: Day 2, Day 8, Day 15, Day 29 and Day 60

InterventionLiters per hour (Median)
Participants in TQ Only Arms2.96

Time to Fever Clearance

Fever clearance time was defined as time from first dose of treatment to the time when body temperature falls to normal within Study Days 1-4 and remains normal for at least 48 hours up to the Day 8 visit. Fever clearance was considered to have been achieved once an initial temperature of more than 37.40 degree Celsius is reduced to a value less than or equal to 37.40 degree Celsius and in the absence of value more than 37.40 degree Celsius in the following 48 hours up to the Day 8 visit. The time taken to achieve fever clearance was analyzed using Kaplan Meier Methodology. The median fever clearance time along with 95% confidence interval has been presented for each treatment group. (NCT01376167)
Timeframe: Up to Day 180

InterventionHours (Median)
CQ Only7
TQ + CQ7
PQ + CQ8

Time to Parasite Clearance

Parasite clearance time was defined as time needed to clear asexual parasite from the blood that is, parasite numbers falling below the limit of detection in the thick blood smear and remaining undetectable after 6 to 12 hours. The time taken to achieve parasite clearance was analyzed using Kaplan Meier Methodology. The median parasite clearance time along with 95% confidence interval has been presented for each treatment group. (NCT01376167)
Timeframe: Up to Day 180

InterventionHours (Median)
CQ Only43
TQ + CQ45
PQ + CQ42

Time to Recurrence of P Vivax Malaria

Recurrence was defined as the first confirmed presence of P vivax asexual stage parasites after clearance of initial parasitemia following CQ treatment. Time to recurrence was defined as the time (in days) from initial parasite clearance to recurrence. The time to recurrence was analyzed by the Kaplan-Meier method. NA indicates data was not available due to insufficient number of participants with events during the follow up period in the study. The median number of days to recurrence along with 95% confidence interval has been presented for each treatment group. (NCT01376167)
Timeframe: Up to Day 180

InterventionDays (Median)
CQ Only86
TQ + CQNA
PQ + CQNA

Volume of Distribution (Vc/F) of TQ

Apparent population central volume of distribution of TQ (NCT01376167)
Timeframe: Day 2, Day 8, Day 15, Day 29 and Day 60

InterventionLiters (Median)
Participants in TQ Only Arms915

Change From Baseline in Percent Methemoglobin

Methemoglobin assessment was made with the aid of a non-invasive signal extraction pulse CO-Oximeter handheld machine (Masimo). The change from Baseline in percent methemoglobin by treatment, time and sex has been summarized. The last assessment performed prior to the first dose of study medication (CQ or randomized treatment) was considered as Baseline. Change from Baseline was calculated as the post baseline assessment minus the Baseline assessment for percent methemoglobin. Only those participants with data available at the specified data points were analyzed. (NCT01376167)
Timeframe: Baseline and up to Day 120

,,
InterventionPercent Methemoglobin (Mean)
Day 2, MaleDay 2, FemaleDay 3, MaleDay 3, FemaleDay 5, MaleDay 5, FemaleDay 8, MaleDay 8, FemaleDay 11, MaleDay 11, FemaleDay 15, MaleDay 15, FemaleDay 22, MaleDay 22, FemaleDay 29, MaleDay 29, FemaleDay 60, MaleDay 60, FemaleDay 120, MaleDay 120, Female
CQ Only-0.18-0.22-0.15-0.20-0.28-0.20-0.12-0.16-0.07-0.130.12-0.080.07-0.05-0.10-0.180.440.190.200.10
PQ + CQ-0.10-0.01-0.020.111.280.903.012.583.613.413.513.631.961.860.580.490.200.160.370.37
TQ + CQ-0.030.10-0.010.260.421.370.982.041.172.130.941.670.540.930.230.24-0.100.030.07-0.03

Cost Associated With Recurrence Episode of P Vivax Malaria

Health outcomes were evaluated based on the total costs spent on treatment, transport, medication and tests. The cost was summarized according to the place at which the participant went to for care (drug shop, trial clinic, other clinic, hospital (inpatient/outpatient), traditional healer, other). The reported costs by type and by site has been summarized. Where costs have not been reported at a visit, the number of participants analyzed is given as 0. Only those participants with data available at the specified data points were analyzed. (NCT01376167)
Timeframe: Up to Day 180

InterventionUS Dollars (USD) (Mean)
Brazil (Drug shop for care)Brazil (Enrollment clinic for care)Brazil (other location for care)Peru (Drug shop for care)Peru (Enrollment clinic for care)Peru (Attended another clinic)Peru (Other location for care)Thailand (Drug shop for care)Thailand (Enrollment clinic for care)Thailand (In-hospital care)
First Malaria Recurrence4.766.174.231.478.782.710.724.6019.156.13

Cost Associated With Recurrence Episode of P Vivax Malaria

Health outcomes were evaluated based on the total costs spent on treatment, transport, medication and tests. The cost was summarized according to the place at which the participant went to for care (drug shop, trial clinic, other clinic, hospital (inpatient/outpatient), traditional healer, other). The reported costs by type and by site has been summarized. Where costs have not been reported at a visit, the number of participants analyzed is given as 0. Only those participants with data available at the specified data points were analyzed. (NCT01376167)
Timeframe: Up to Day 180

InterventionUS Dollars (USD) (Mean)
Brazil (Enrollment clinic for care)Peru (Enrollment clinic for care)Peru (Attended another clinic)Peru (Other location for care)
First Malaria Recurrence Follow-up6.158.543.941.30

Cost Incurred With Purchase of Medications Associated With Recurrence Episode of Malaria

"Health outcomes were evaluated based on the cost of medications purchased. The reported total medication cost for paracetamol associated with recurrence episode of P vivax malaria has been reported by site. Where costs have not been reported at a visit, the number of participants analyzed is given as 0. Medications recorded as Other and medications without costs are excluded from the analysis. Only those participants with data available at the specified data points were analyzed." (NCT01376167)
Timeframe: Up to Day 180

InterventionUSD (Mean)
Peru, n=23, 3
First Malaria Recurrence Follow-up0.32

Cost Incurred With Purchase of Medications Associated With Recurrence Episode of Malaria

"Health outcomes were evaluated based on the cost of medications purchased. The reported total medication cost for paracetamol associated with recurrence episode of P vivax malaria has been reported by site. Where costs have not been reported at a visit, the number of participants analyzed is given as 0. Medications recorded as Other and medications without costs are excluded from the analysis. Only those participants with data available at the specified data points were analyzed." (NCT01376167)
Timeframe: Up to Day 180

InterventionUSD (Mean)
Peru, n=23, 3Brazil, n=6, 0
First Malaria Recurrence0.491.70

Incidence of Visual Field Abnormalities Based on Best Corrected Visual Acuity Test Scores

Ophthalmic assessments were carried out at pre-qualified sites (Manaus) prior to randomization and at Days 29 and 90 and at withdrawal. Assessments were carried out at Day 180 if the Day 90 assessments showed abnormalities. The last assessment performed on the day of randomization or earlier was considered Baseline. Best corrected visual acuity was assessed individually for each eye. Scores were recorded as a ratio. The values were used to derive a logMAR score for statistical analysis where logMAR=-1x log10 (ratio score). The mean and standard deviation of logMAR score for each treatment group has been summarized. High scores were associated with worse vision, and low scores with better vision. Only those participants with data available at the specified data points were analyzed. (NCT01376167)
Timeframe: Up to Day 180

InterventionlogMAR scores (Mean)
Baseline; right eyeBaseline; left eyeDay 29; right eyeDay 29; left eyeDay 90; right eyeDay 90; left eye
CQ Only0.0410.0480.0390.0320.0440.041

Incidence of Visual Field Abnormalities Based on Best Corrected Visual Acuity Test Scores

Ophthalmic assessments were carried out at pre-qualified sites (Manaus) prior to randomization and at Days 29 and 90 and at withdrawal. Assessments were carried out at Day 180 if the Day 90 assessments showed abnormalities. The last assessment performed on the day of randomization or earlier was considered Baseline. Best corrected visual acuity was assessed individually for each eye. Scores were recorded as a ratio. The values were used to derive a logMAR score for statistical analysis where logMAR=-1x log10 (ratio score). The mean and standard deviation of logMAR score for each treatment group has been summarized. High scores were associated with worse vision, and low scores with better vision. Only those participants with data available at the specified data points were analyzed. (NCT01376167)
Timeframe: Up to Day 180

,
InterventionlogMAR scores (Mean)
Baseline; right eyeBaseline; left eyeDay 29; right eyeDay 29; left eyeDay 90; right eyeDay 90; left eyeDay 180; right eyeDay 180; left eye
PQ + CQ0.0290.0480.0210.0450.0160.0410.0000.000
TQ + CQ0.0460.0390.0490.0320.0380.0280.0330.033

Number of Participants With Action Taken to Treat Recurrence Episode of P Vivax Malaria

Health outcomes were evaluated based on the actions taken by the participants to treat recurrence episode of P vivax malaria. The reported action taken by site is summarized. Where no action by site have been reported at a visit, the number of participants analyzed is given as 0. Only those participants with data available at the specified data points were analyzed. (NCT01376167)
Timeframe: Up to Day 180

InterventionParticipants (Number)
Brazil, NothingBrazil, Drug shopBrazil, Trial clinicBrazil, OtherCambodia, NothingEthiopia, NothingEthiopia, Another clinicEthiopia, OtherEthiopia, Trial clinicPeru, NothingPeru, Drug shopPeru, Trial clinicPeru, Another clinicPeru, OtherThailand, NothingThailand, Drug shopThailand, Trial clinicThailand, In hospital
First Malaria Recurrence Follow-up507601413001006354116000

Number of Participants With Action Taken to Treat Recurrence Episode of P Vivax Malaria

Health outcomes were evaluated based on the actions taken by the participants to treat recurrence episode of P vivax malaria. The reported action taken by site is summarized. Where no action by site have been reported at a visit, the number of participants analyzed is given as 0. Only those participants with data available at the specified data points were analyzed. (NCT01376167)
Timeframe: Up to Day 180

InterventionParticipants (Number)
Brazil, NothingBrazil, Drug shopBrazil, Trial clinicBrazil, OtherCambodia, NothingEthiopia, NothingEthiopia, Another clinicEthiopia, OtherEthiopia, Trial clinicPeru, NothingPeru, Drug shopPeru, Trial clinicPeru, Another clinicPeru, OtherPhilippines, NothingThailand, NothingThailand, Drug shopThailand, Trial clinicThailand, In hospital
First Malaria Recurrence212622131211018611015111131

Number of Participants With Clinical Chemistry Laboratory Data Outside the Reference Range

Blood samples were collected for the evaluation of clinical chemistry parameters including Alanine Aminotransferase (ALT), Alkaline Phosphatase (Alk. Phos), Aspartate Aminotransferase (AST), bilirubin, creatine kinase, creatinine, glomerular filtration rate (GFR), indirect bilirubin and urea. The number of participants with clinical chemistry laboratory data outside the extended normal range (F3) was presented. The upper and lower limits for F3 range were defined by multiplying the normal range limits by different factors. High and low indicated that the participants had values flagged as high and low respectively for the particular parameter any time on-treatment. Only those participants with data available at the specified data points were analyzed. (NCT01376167)
Timeframe: Up to Day 120

,,
InterventionParticipants (Number)
ALT, HighAlk Phos, HighAST, HighBilirubin, HighCreatine kinase, HighCreatinine, HighGFR, LowIndirect bilirubinUrea, High
CQ Only1135188001142
PQ + CQ51212800846
TQ + CQ1017235112285

Number of Participants With Gastrointestinal Disorders

Gastrointestinal tolerability was analyzed by the number of par experiencing gastrointestinal disorders such as abdominal pain, heartburn, diarrhea, constipation, nausea, and vomiting. The number of participants with gastrointestinal disorders for each treatment group has been summarized. (NCT01376167)
Timeframe: Up to Day 180

,,
InterventionParticipants (Number)
NauseaVomitingAbdominal pain upperDiarrhoeaAbdominal painDyspepsia
CQ Only12913655
PQ + CQ9117562
TQ + CQ2122111586

Number of Participants With Hematology Laboratory Data Outside the Reference Range

Blood samples were collected for the evaluation of hematology parameters including eosinophils, leukocytes, lymphocytes, neutrophils, platelets, reticulocytes and methemoglobin. The number of participants with hematology laboratory data outside the extended normal range (F3) was presented. The upper and lower limits for F3 range were defined by multiplying the normal range limits by different factors. High and low indicated that the participants had values flagged as high and low respectively for the particular parameter any time on-treatment. Only those participants with data available at the specified data points were analyzed. (NCT01376167)
Timeframe: Up to Day 120

,,
InterventionParticipants (Number)
Blood eosinophils, HighBlood leukocytes, LowBlood lymphocytes, LowBlood lymphocytes, HighBlood neutrophils, LowBlood platelets, LowBlood reticulocytes, HighMethemoglobin, High
CQ Only180723214724
PQ + CQ2820137158511
TQ + CQ3834325351415

Number of Participants With Hemoglobin Decline From Baseline Over First 29 Days

Glucose-6-phosphate dehydrogenase deficiency (G6PD) deficiency is known to be a risk factor for hemolysis in participants treated with 8-aminoquinolines. Blood samples were collected for the evaluation of hemoglobin levels. Hemoglobin decreases of >=30% or >3 grams/deciliter (g/dL) from Baseline; or, an overall drop in hemoglobin below 6.0 g/dL in the first 15 days of the study were considered as protocol defined serious adverse events (SAEs). Number of participants with maximum hemoglobin decline from Baseline over first 29 days of study has been summarized. Safety Population consisted of all randomized participants who received at least one dose of study medication. (NCT01376167)
Timeframe: Baseline and up to Day 29

,,
InterventionParticipants (Number)
<=20 grams/liter (g/L)>20g/L to <=30 g/L>30 g/L or >=30%
CQ Only120112
PQ + CQ114123
TQ + CQ2143114

Number of Participants With Keratopathy

Ophthalmic assessments were carried out at pre-qualified sites (Manaus) prior to randomization and at Days 29 and 90 and at withdrawal. Assessments were carried out at Day 180 if the Day 90 assessments showed abnormalities. The last assessment performed on the day of randomization or earlier was considered Baseline. The number of participants displaying keratopathy in each eye was summarized for each visit. The number of participants with new keratopathy at any time post Baseline was also reported. Ophthalmic Safety Population comprised of all participants in the Safety Population who have results from any eye assessments. Only those participants with data available at the specified data points were analyzed. (NCT01376167)
Timeframe: Up to Day 180

InterventionParticipants (Number)
Baseline; right eyeBaseline; left eyeDay 1; right eyeDay 1; left eyeDay 29; right eyeDay 29; left eyeDay 90; right eyeDay 90; left eyeAny time post Baseline; right eyeAny time post Baseline; left eye
CQ Only0000000000

Number of Participants With Keratopathy

Ophthalmic assessments were carried out at pre-qualified sites (Manaus) prior to randomization and at Days 29 and 90 and at withdrawal. Assessments were carried out at Day 180 if the Day 90 assessments showed abnormalities. The last assessment performed on the day of randomization or earlier was considered Baseline. The number of participants displaying keratopathy in each eye was summarized for each visit. The number of participants with new keratopathy at any time post Baseline was also reported. Ophthalmic Safety Population comprised of all participants in the Safety Population who have results from any eye assessments. Only those participants with data available at the specified data points were analyzed. (NCT01376167)
Timeframe: Up to Day 180

,
InterventionParticipants (Number)
Baseline; right eyeBaseline; left eyeDay 1; right eyeDay 1; left eyeDay 29; right eyeDay 29; left eyeDay 90; right eyeDay 90; left eyeDay 180; right eyeDay 180; left eyeAny time post Baseline; right eyeAny time post Baseline; left eye
PQ + CQ000000000000
TQ + CQ000000100010

Number of Participants With Retinal Changes From Baseline

Ophthalmic assessments were carried out at pre-qualified sites (Manaus) prior to randomization and at Days 29 and 90 and at withdrawal. Assessments were carried out at Day 180 if the Day 90 assessments showed abnormalities. The last assessment performed on the day of randomization or earlier was considered Baseline. Change from Baseline was calculated as the post Baseline assessment minus the Baseline assessment. The number of participants with definite retinal change and questionable (ques) retinal change from Baseline was presented. Only those participants with data available at the specified data points were analyzed. (NCT01376167)
Timeframe: Baseline and up to Day 180

,
InterventionParticipants (Number)
Day 29, Definite change, right eyeDay 29, Ques change, right eyeDay 29, Definite change, left eyeDay 29, Ques change, left eyeDay 90, Definite change, right eyeDay 90, Ques change, right eyeDay 90, Definite change, left eyeDay 90, Ques change, left eyeDay 180, Definite change, right eyeDay 180, Ques change, right eyeDay 180, Definite change, left eyeDay 180, Ques change, left eye
CQ Only101010100000
TQ + CQ000010110000

Number of Participants With Retinal Changes From Baseline

Ophthalmic assessments were carried out at pre-qualified sites (Manaus) prior to randomization and at Days 29 and 90 and at withdrawal. Assessments were carried out at Day 180 if the Day 90 assessments showed abnormalities. The last assessment performed on the day of randomization or earlier was considered Baseline. Change from Baseline was calculated as the post Baseline assessment minus the Baseline assessment. The number of participants with definite retinal change and questionable (ques) retinal change from Baseline was presented. Only those participants with data available at the specified data points were analyzed. (NCT01376167)
Timeframe: Baseline and up to Day 180

InterventionParticipants (Number)
Day 29, Definite change, right eyeDay 29, Ques change, right eyeDay 29, Definite change, left eyeDay 29, Ques change, left eyeDay 90, Definite change, right eyeDay 90, Ques change, right eyeDay 90, Definite change, left eyeDay 90, Ques change, left eye
PQ + CQ00001102

Number of Participants With TEAEs and Serious TEAEs

An AE is defined as any untoward medical occurrence in a participant under clinical investigation, temporarily associated with the use of a medicinal product, whether or not considered related to the medicinal product. SAE is defined as any untoward medical occurrence that, at any dose results in death, is life-threatening, requires hospitalization or prolongation of existing hospitalization, results in disability/incapacity, is a congenital anomaly/ birth defect, other situations and is associated with possible drug induced liver injury with hyperbilirubinemia. TEAEs is defined as AEs with an onset date and time on or after that of the start of first dose of study medication (including CQ). Number of participants with TEAEs and serious TEAEs have been presented. (NCT01376167)
Timeframe: Up to Day 180

,,
InterventionParticipants (Number)
TEAEsSerious TEAEs
CQ Only866
PQ + CQ764
TQ + CQ16421

Number of Participants With TEAEs by Maximum Intensity

An AE is defined as any untoward medical occurrence in a participant under clinical investigation, temporarily associated with the use of a medicinal product, whether or not considered related to the medicinal product. TEAE is defined as AEs with an onset date and time on or after that of the start of first dose of study medication (including CQ). Number of participants with AEs based on severity has been presented. (NCT01376167)
Timeframe: Up to Day 180

,,
InterventionParticipants (Number)
Mild or Grade 1Moderate or Grade 2Severe or Grade 3Grade 4Grade 5
CQ Only3052310
PQ + CQ3837100
TQ + CQ7089201

Number of Participants With Treatment Emergent Adverse Events (TEAEs) Potentially Related to Hemoglobin Decrease

TEAEs are defined as adverse events (AEs) with an onset date and time on or after that of the start of first dose of study medication (including CQ). The number of participants with TEAEs potentially related to hemoglobin decrease has been presented. (NCT01376167)
Timeframe: Up to Day 180

,,
InterventionParticipants (Number)
Haemoglobin decreasedFatigueHyperbilirubinaemiaPallor
CQ Only2210
PQ + CQ2000
TQ + CQ14101

Time Lost by Participants or Care Givers From Normal Occupation

Health outcomes were evaluated based on total time lost by participants or care givers due to an episode of malaria. The reported time lost due to recurrence episode of P vivax malaria has been summarized by category and by site. Where categories by site have not been reported at a visit, the number of participants analyzed is given as 0. Only those participants with data available at the specified data points were analyzed. (NCT01376167)
Timeframe: Up to Day 180

InterventionDays (Number)
Brazil, HouseworkBrazil, FarmingBrazil, paid employmentBrazil, OtherCambodia, FarmingEthiopia, HouseworkEthiopia, FarmingEthiopia, StudentEthiopia, Paid employmentEthiopia, OtherPeru, HouseworkPeru, FarmingPeru, StudentPeru, Paid employmentPeru, OtherThailand, paid employmentThailand, Other
First Malaria Recurrence Follow-up00052433047292868.53200

Time Lost by Participants or Care Givers From Normal Occupation

Health outcomes were evaluated based on total time lost by participants or care givers due to an episode of malaria. The reported time lost due to recurrence episode of P vivax malaria has been summarized by category and by site. Where categories by site have not been reported at a visit, the number of participants analyzed is given as 0. Only those participants with data available at the specified data points were analyzed. (NCT01376167)
Timeframe: Up to Day 180

InterventionDays (Number)
Brazil, HouseworkBrazil, FarmingBrazil, paid employmentBrazil, OtherCambodia, FarmingEthiopia, HouseworkEthiopia, FarmingEthiopia, StudentEthiopia, Paid employmentEthiopia, OtherPeru, HouseworkPeru, FarmingPeru, StudentPeru, Paid employmentPeru, OtherPhilippines, FarmingThailand, paid employmentThailand, Other
First Malaria Recurrence18831742.5321241916260201

Cost Associated With a Hemolysis Event

Health outcomes were evaluated based on cost incurred due to clinically relevant hemolysis. The total cost was evaluated based on the amount spent on treatment, transport, medication and test. The costs associated with hemolysis event has been presented. The aim of this outcome measure was to determine the cost to a participant due to an event of hemolysis, regardless of treatment received in the study. It was not expected there would be major cost differences with hemoglobin decrease between the treatment arms. This was pre-specified in the statistical analysis plan. (NCT02216123)
Timeframe: Up to Day 180

InterventionUSD (Mean)
Participants With Clinically Relevant Hemolysis9.174

Cost Incurred With Purchase of Medications Associated With Hemolysis Event

"Health outcomes were evaluated based on the cost of medications purchased. The total medication cost associated with hemolysis event has been presented. Medications recorded as Other and medications without costs are excluded from the analysis. The aim of this outcome measure was to determine the cost to a participant due to an event of hemolysis, regardless of treatment received in the study. It was not expected there would be major cost differences with hemoglobin decrease between the treatment arms. This was pre-specified in the statistical analysis plan." (NCT02216123)
Timeframe: Up to Day 180

InterventionUSD (Mean)
Participants With Clinically Relevant Hemolysis0

Number of Participants or Care Givers Who Had Taken Time Off From Normal Occupation Due to a Hemolysis Event

Health outcomes were evaluated based on total time lost by participants or care givers due to a hemolysis event. The number of participants or care givers who took days off from work due to a hemolysis event has been presented based on the normal occupation. The aim of this outcome measure was to determine the time taken off by participants due to an event of hemolysis, regardless of treatment received in the study. It was not expected there would be major differences in time taken off by participants with hemoglobin decrease between the treatment arms. This was pre-specified in the statistical analysis plan. (NCT02216123)
Timeframe: Up to Day 180

InterventionParticipants (Number)
Participants With Clinically Relevant Hemolysis0

Number of Participants With Action Taken to Treat a Hemolysis Event

Health outcomes were evaluated based on the actions taken by the participants to treat hemolysis events. The number of participants in Brazil who attended the trial clinic to treat a hemolysis event has been presented. The aim of this outcome measure was to determine the action taken by a participant due to an event of hemolysis, regardless of treatment received in the study. It was not expected there would be major differences in action taken by the participants with hemoglobin decrease between the treatment arms. This was pre-specified in the statistical analysis plan. (NCT02216123)
Timeframe: Up to Day 180

InterventionParticipants (Number)
Participants With Clinically Relevant Hemolysis1

Number of Participants With P. Falciparum

Microscopic blood slides (two thick film and one thin film slide) were prepared and examined for asexual parasite count. The number of participants with positive P. falciparum asexual parasite count post Baseline has been summarized for each treatment arm. (NCT02216123)
Timeframe: Up to Day 180

InterventionParticipants (Number)
TQ+CQ4
PQ+CQ3

Number of Participants With Recrudescence

Recrudescence is defined as any P. vivax parasitemia occurring on or before Day 32 (that is, blood stage treatment failure). A participant was considered to have had a recrudescence if both of the following were true: a) Participant had a positive P. vivax asexual parasite count at Baseline and demonstrated clearance (that is, did not have two negative asexual P. vivax parasite counts, with at least 6 hours between the counts, and no positive counts in the interval). b) Participant had a positive genetically homologous asexual P. vivax parasite count, after their zero count in Days 1 to 5, but on or before Study Day 32. The number of participants with recrudescence before Study Day 33 has been presented. (NCT02216123)
Timeframe: Up to Day 32

InterventionParticipants (Number)
TQ+CQ0
PQ+CQ0

Oral Clearance (CL/F) of TQ

Apparent population oral clearance of TQ (NCT02216123)
Timeframe: Day 2, Day 3, Day 8, Day 15, Day 29, Day 60 and Day 180

InterventionLiters per hour (Median)
Participants in TQ Only Arms2.96

Percentage of Participants With Clinically Relevant Hemolysis.

Clinically relevant hemolysis is defined as a decrease in hemoglobin of >=30% or >3 grams per deciliter (g/dL) from Baseline; or, an overall drop in hemoglobin below 6.0 g/dL at any visit after the first dose of study medication. The percentage of participants with clinically relevant hemolysis has been summarized. Safety Population comprised of all randomized participants who received at least one dose of blinded study medication. (NCT02216123)
Timeframe: Up to Day 180

InterventionPercentage of participants (Number)
TQ+CQ2.41
PQ+CQ1.18

Rate of Relapse-free Efficacy at Four Months Post Dose

A participant was considered to have demonstrated recurrence-free efficacy at 4 months if: a) Participant had non-zero P. vivax asexual parasite count at Baseline. b) Participant showed initial clearance of P. vivax parasitemia. c) Participant had no positive asexual P. vivax parasite count at any assessment prior to or on Study Day 130 following initial parasite clearance. d) Participant did not take a concomitant medication with anti-malarial activity at any point between Study Day 1 and their last parasite assessment after Study Day 109 (up to and including Study Day 130). e) Participant is parasite-free at 4 months. The rate of relapse-free efficacy was estimated by Kaplan-Meier methodology. The percentage of participants who were relapse-free at 4 months post dose has been presented along with 95% confidence interval. (NCT02216123)
Timeframe: 4 months post dose

InterventionPercentage of participants (Number)
TQ+CQ82.3
PQ+CQ79.7

Rate of Relapse-free Efficacy at Six Months Post Dose

A participant was considered to have demonstrated relapse-free efficacy at 6 months if: a) Participant had non-zero P. vivax asexual parasite count at Baseline. b) Participant showed initial clearance of P. vivax parasitemia defined as two negative asexual P. vivax parasite counts, with at least 6 hours between the counts, and no positive counts in the interval. c) Participant had no positive asexual P. vivax parasite count at any assessment prior to or on Study Day 201 following initial parasite clearance. d) Participant did not take a concomitant medication with anti-malarial activity at any point between Study Day 1 and their last parasite assessment. e) Participant is parasite-free at 6 months. The rate of relapse-free efficacy was estimated by Kaplan-Meier methodology. The percentage of participants who were relapse-free at 6 months post dose has been presented along with 95% confidence interval. (NCT02216123)
Timeframe: 6 months post dose

InterventionPercentage of participants (Number)
TQ+CQ72.7
PQ+CQ75.1

Time to Fever Clearance

Fever clearance time is defined as the time from first dose of treatment to the time when body temperature falls to normal within Study Days 1-4 and remains normal for at least 48 hours up to the Day 8 visit. Fever clearance was considered to have been achieved once an initial temperature of more than 37.4 degree Celsius is reduced to a value less than or equal to 37.4 degree Celsius, in the absence of value more than 37.4 degree Celsius in the following 48 hours up to the Day 8 visit. The time taken to achieve fever clearance was analyzed by Kaplan-Meier method. (NCT02216123)
Timeframe: Up to Day 9

InterventionHours (Median)
TQ+CQ10
PQ+CQ13

Time to Gametocyte Clearance

Gametocyte clearance time is defined as time from first dose until the first slide that was gametocyte negative and remained so at the next slide reading. The time taken to achieve gametocyte clearance was analyzed by Kaplan-Meier method. (NCT02216123)
Timeframe: Up to Day 180

InterventionHours (Median)
TQ+CQ38
PQ+CQ41

Time to Parasite Clearance

Parasite clearance time is defined as time needed to clear asexual parasite from the blood that is, parasite numbers falling below the limit of detection in the thick blood smear and remaining undetectable after 6 to 12 hours later. The time to achieve parasite clearance was analyzed by Kaplan-Meier methodology. The median parasite clearance time along with 95% confidence interval has been presented for each treatment group. (NCT02216123)
Timeframe: Up to Day 180

InterventionHours (Median)
TQ+CQ41
PQ+CQ44

Time to Relapse of P. Vivax Malaria

Relapse is defined by a positive blood smear with or without vivax symptoms. Relapse is described as any recurrence of malaria that occurred after Day 32 of the study. The time to relapse was analyzed by the Kaplan-Meier method. The median number of days to relapse along with 95% confidence interval has been presented for each treatment group. (NCT02216123)
Timeframe: Up to Day 180

InterventionDays (Median)
TQ+CQNA
PQ+CQNA

Volume of Distribution (Vc/F) of TQ

Apparent population central volume of distribution of TQ (NCT02216123)
Timeframe: Day 2, Day 3, Day 8, Day 15, Day 29, Day 60 and Day 180

InterventionLiters (Median)
Participants in TQ Only Arms915

Change From Baseline in Percent Methemoglobin

Methemoglbin is an oxidized and inactive form of hemoglobin. Methemoglobin assessment was made with the aid of a non-invasive signal extraction pulse CO-Oximeter handheld machine. The change from Baseline in percent methemoglobin by treatment, time and sex has been summarized. The latest pre-treatment assessment where treatment is their first dose of study medication (CQ/PQ/TQ/Placebo) was considered as Baseline value. Change from Baseline is the value at post dose visit minus the Baseline value. Only those participants with data available at the specified data points were analyzed (represented by n=X in category title). (NCT02216123)
Timeframe: Baseline and up to Day 120

,
InterventionPercent change (Mean)
Day 2, Male, n=114, 53Day 2, Female, n=52, 32Day 3, Male, n=114, 53Day 3, Female, n=52, 32Day 5, Male, n=113, 53Day 5, Female, n=52, 32Day 8, Male, n=112, 52Day 8, Female, n=52, 32Day 11, Male, n=112, 52Day 11, Female, n=51, 32Day 15, Male, n=113, 52Day 15, Female, n=52, 32Day 22, Male, n=112, 52Day 22, Female, n=52, 32Day 29, Male, n=111, 52Day 29, Female, n=52, 32Day 60, Male, n=107, 51Day 60, Female, n=52, 32Day 120, Male, n=109, 50Day 120, Female, n=50, 31
PQ+CQ0.02-0.060.030.170.891.322.632.813.303.443.263.611.582.300.460.840.200.14-0.010.04
TQ+CQ0.02-0.160.180.080.770.631.221.001.161.041.010.810.610.320.24-0.020.05-0.090.060.14

Change From Baseline in Pulse Rate

Vital signs were measured twice a day on Days 1 through 3, at least 4 hours apart, and immediately prior to PK measurements. The mean and standard deviation of pulse rate has been presented. The values presented does not include Day 3 assessments for participant number 570. Baseline value is defined as the latest pre-treatment assessment where treatment is their first dose of study medication (CQ/PQ/TQ/Placebo). Change from Baseline is the value at post dose minus Baseline value. Only those participants with data available at the specified data points were analyzed (represented by n=X in category title). (NCT02216123)
Timeframe: Baseline and up to Day 180

,
Interventionbeats per minute (Mean)
Day 1 assessment 4; n=161, 84Day 2 assessment 1; n=166, 85Day 2 assessment 4; n=166, 85Day 3 assessment 1; n=166, 83Day 3 assessment 4; n=166, 82Day 8; n=164, 84Day 11; n=163, 84Day15; n=165, 84Day 22; n=164, 84Day 29; n=163, 84Day 60; n=160, 83Day 90; n=160, 82Day 120; n=159, 81Day 150; n=161, 82Day180; n=160, 83
PQ+CQ-9.3-9.9-11.8-18.2-17.5-14.6-15.5-16.9-16.8-17.5-18.5-18.6-19.1-17.9-18.3
TQ+CQ-10.8-9.9-11.9-15.1-16.5-12.7-13.4-13.5-14.7-16.9-16.7-16.3-16.7-16.8-18.0

Change From Baseline in Systolic Blood Pressure (SBP), Diastolic Blood Pressure (DBP) and Mean Arterial Pressure (MAP)

Vital signs were measured twice a day on Days 1 through 3, at least 4 hours apart, and immediately prior to pharmacokinetic (PK) measurements. MAP was calculated as the sum of SBP and two times DBP divided by 3. The mean and standard deviation of SBP, DBP and MAP has been presented. The values presented does not include Day 3 assessments for participant number 570. Baseline value is defined as the latest pre-treatment assessment where treatment is their first dose of study medication (CQ/PQ/TQ/Placebo). Change from Baseline is the value at post dose minus Baseline value. Only those participants with data available at the specified data points were analyzed (represented by n=X in category title). (NCT02216123)
Timeframe: Baseline and up to Day 180

,
Interventionmillimeter of mercury (mmHg) (Mean)
SBP, Day 1 assessment 4; n=161, 84SBP, Day 2 assessment 1; n=166, 85SBP, Day 2 assessment 4; n=166, 85SBP, Day 3 assessment 1; n=166, 83SBP, Day 3 assessment 4; n=166, 82SBP, Day 8; n=164, 84SBP, Day 11; n=163, 84SBP, Day15; n=165, 84SBP, Day 22; n=164, 84SBP, Day 29; n=163, 84SBP, Day 60; n=160, 83SBP, Day 90; n=160, 82SBP, Day 120; n=159, 81SBP, Day 150; n=161, 82SBP, Day180; n=160, 83DBP, Day 1 assessment 4; n=161, 84DBP, Day 2 assessment 1; n=166, 85DBP, Day 2 assessment 4; n=166, 85DBP, Day 3 assessment 1; n=166, 83DBP, Day 3 assessment 4; n=166, 82DBP, Day 8; n=164, 84DBP, Day 11; n=163, 84DBP, Day15; n=165, 84DBP, Day 22; n=164, 84DBP, Day 29; n=163, 84DBP, Day 60; n=160, 83DBP, Day 90; n=160, 82DBP, Day 120; n=159, 81DBP, Day 150; n=161, 82DBP, Day180; n=160, 83MAP, Day 1 assessment 4; n=161, 84MAP, Day 2 assessment 1; n=166, 85MAP, Day 2 assessment 4; n=166, 85MAP, Day 3 assessment 1; n=166, 83MAP, Day 3 assessment 4; n=166, 82MAP, Day 8; n=164, 84MAP, Day 11; n=163, 84MAP, Day15; n=165, 84MAP, Day 22; n=164, 84MAP, Day 29; n=163, 84MAP, Day 60; n=160, 83MAP, Day 90; n=160, 82MAP, Day 120; n=159, 81MAP, Day 150; n=161, 82MAP, Day180; n=160, 83
PQ+CQ-0.9-2.3-2.7-2.1-2.20.81.22.52.94.44.35.33.14.95.7-1.5-2.2-2.6-1.3-1.91.1-0.50.41.31.51.93.52.44.13.7-1.3-2.2-2.6-1.6-2.01.00.11.11.82.42.74.12.64.44.4
TQ+CQ1.20.4-0.8-0.6-2.72.21.33.23.32.64.43.83.84.43.71.1-0.1-0.8-0.2-1.90.9-0.01.51.20.93.12.73.33.22.91.10.0-0.8-0.3-2.21.30.42.01.91.53.53.13.53.63.2

Change From Baseline in Temperature

Vital signs were performed twice a day on Days 1 through 3, at least 4 hours apart, and immediately prior to PK measurements. The mean and standard deviation of pulse rate has been presented. The values presented does not include Day 3 assessments for participant number 570. Baseline value is defined as the latest pre-treatment assessment where treatment is their first dose of study medication (CQ/PQ/TQ/Placebo). Change from Baseline is the value at post dose minus Baseline value. Only those participants with data available at the specified data points were analyzed (represented by n=X in category title). (NCT02216123)
Timeframe: Baseline and up to Day 180

,
InterventionCelsius (Mean)
Day 1 assessment 4; n=161, 84Day 2 assessment 1; n=166, 85Day 2 assessment 4; n=166, 85Day 3 assessment 1; n=166, 83Day 3 assessment 4; n=166, 82Day 8; n=164, 84Day 11; n=163, 84Day15; n=165, 84Day 22; n=164, 84Day 29; n=163, 84Day 60; n=160, 83Day 90; n=160, 82Day 120; n=159, 81Day 150; n=161, 82Day180; n=160, 83
PQ+CQ-0.5-0.6-0.6-0.9-1.0-0.9-0.9-1.0-1.0-1.0-1.0-1.0-0.9-1.0-1.0
TQ+CQ-0.6-0.6-0.6-1.0-1.0-1.0-1.0-0.9-1.0-1.0-1.0-1.0-1.0-1.0-1.0

Cost Associated With Relapse Episode of P Vivax Malaria

Health outcomes were evaluated based on the total costs spent on treatment, transport, medication and tests. The cost was summarized according to the place at which the participant went to for care (drug shop, trial clinic, other clinic, hospital emergency center, other). The costs associated with a relapse episode of P. vivax malaria has been presented. Participants may be represented in more than one category, so the total number of participants may be less than the number quoted. Only those participants with data available at the specified data points were analyzed (represented by n=X in category title). (NCT02216123)
Timeframe: Up to Day 180

InterventionUS Dollars (USD) (Mean)
Brazil; enrollment clinic for care; n=19, 17Colombia; hospital emergency center; n=1,1Peru; enrollment clinic for care; n=32, 33Peru; attended another clinic; n=8, 30Thailand; enrollment clinic for care; n=0, 1Vietnam; drug shop for care;n=1, 2Vietnam; attended another clinic; n=0, 1
First Malaria Relapse Follow-up8.03216.7758.8153.9591.5342.8090.936

Cost Associated With Relapse Episode of P Vivax Malaria

Health outcomes were evaluated based on the total costs spent on treatment, transport, medication and tests. The cost was summarized according to the place at which the participant went to for care (drug shop, trial clinic, other clinic, hospital emergency center, other). The costs associated with a relapse episode of P. vivax malaria has been presented. Participants may be represented in more than one category, so the total number of participants may be less than the number quoted. Only those participants with data available at the specified data points were analyzed (represented by n=X in category title). (NCT02216123)
Timeframe: Up to Day 180

InterventionUS Dollars (USD) (Mean)
Brazil; enrollment clinic for care; n=19, 17Colombia; enrollment clinic for care; n=1,0Colombia; attended another clinic; n=1,0Colombia; hospital emergency center; n=1,1Peru; enrollment clinic for care; n=32, 33Peru; attended another clinic; n=8, 30Peru; Other; n=8, 0Vietnam; drug shop for care;n=1, 2Vietnam; Other; n=1, 0
First Malaria Relapse8.20842.7764.19416.7759.2441.6770.8180.7021.873

Cost Incurred With Purchase of Medications Associated With Relapse Episode of P. Vivax Malaria

"Health outcomes were evaluated based on the cost of medications purchased. The total medication cost for paracetamol associated with relapse episode of P vivax malaria has been presented. Medications recorded as Other and medications without costs are excluded from the analysis. Only those participants with data available at the specified data points were analyzed (represented by n=X in category title)." (NCT02216123)
Timeframe: Up to Day 180

,
InterventionUSD (Mean)
Colombia; n=2, 1Peru; n=6, 2Vietnam; n=1, 1
First Malaria Relapse2.5160.4910.468
First Malaria Relapse Follow-up4.1940.3272.341

Number of Participants or Care Givers Who Had Taken Time Off From Normal Occupation Due to Relapse Episode of Malaria

Health outcomes were evaluated based on total time lost by participants or care givers due to an episode of malaria. The number of participants or care givers who had taken off from their normal occupation due to relapse episode of P vivax malaria has been presented by country. Participants may be represented in more than one category, so the total number of participants may be less than the number quoted. Only those participants with data available at the specified data points were analyzed (represented by n=X in category title). (NCT02216123)
Timeframe: Up to Day 180

InterventionParticipants (Number)
Brazil; Housework; n=2, 1Brazil; Farming; n=1, 1Brazil; Student; n=1, 1Brazil; Paid employment; n=7, 7Brazil; Other; n=8, 7Colombia; Farming; n=2, 2Colombia; Paid employment; n=1, 1Peru; Housework; n=18, 18Peru, Farming; n=4, 4Peru; Student; n=3, 3Peru; Paid employment; n=1, 1Peru; Other; n=7, 7Thailand; Farming; n=1, 1Vietnam; Farming; n=4, 4Vietnam; Paid employment; n=0, 3
First Malaria Relapse Follow-up0000001154216112

Number of Participants or Care Givers Who Had Taken Time Off From Normal Occupation Due to Relapse Episode of Malaria

Health outcomes were evaluated based on total time lost by participants or care givers due to an episode of malaria. The number of participants or care givers who had taken off from their normal occupation due to relapse episode of P vivax malaria has been presented by country. Participants may be represented in more than one category, so the total number of participants may be less than the number quoted. Only those participants with data available at the specified data points were analyzed (represented by n=X in category title). (NCT02216123)
Timeframe: Up to Day 180

InterventionParticipants (Number)
Brazil; Housework; n=2, 1Brazil; Farming; n=1, 1Brazil; Student; n=1, 1Brazil; Paid employment; n=7, 7Brazil; Other; n=8, 7Colombia; Housework; n=1, 0Colombia; Farming; n=2, 2Colombia; Paid employment; n=1, 1Peru; Housework; n=18, 18Peru, Farming; n=4, 4Peru; Student; n=3, 3Peru; Paid employment; n=1, 1Peru; Other; n=7, 7Thailand; Farming; n=1, 1Vietnam; Farming; n=4, 4
First Malaria Relapse0000010114421713

Number of Participants With Abnormal Urinalysis Dipstick Results

Mid-stream urine was collected and analyzed for bilirubin, glucose, ketones, leukocyte esterase (LE), nitrites, occult blood, proteins and urobilinogen by dipstick method. The number of participants with abnormal urinalysis results (Trace, +, ++, +++, ++++) has been presented. Only those participants with data available at the specified data points were analyzed. (NCT02216123)
Timeframe: Up to Day 120

,
InterventionParticipants (Number)
Bilirubin, Day 1, TraceBilirubin, Day 1, +Bilirubin, Day1, ++Bilirubin, Day 3, +Bilirubin, Day 3, ++Bilirubin, Day 5, TraceBilirubin, Day 5, +Bilirubin, Day 8, +Bilirubin, Day 11, TraceBilirubin, Day 22, TraceBilirubin, Day 22, +Bilirubin, Day 60, TraceBilirubin, Day 60, +Bilirubin, Day 90, +Bilirubin, Day 120, +Glucose, Day 1, +Glucose, Day 1, ++Glucose, Day1, +++Glucose, Day1, ++++Glucose, Day 3, +Glucose, Day 3, ++Glucose, Day 3, +++Glucose, Day 3, ++++Glucose, Day 5, ++Glucose, Day 5, +++Glucose, Day 8, +Glucose, Day 8, ++Glucose, Day 8,+++Glucose, Day 11, TraceGlucose, Day 11, +Glucose, Day 11, ++Glucose, Day 11, +++Glucose, Day 15, ++Glucose, Day 15, +++Glucose, Day 15, ++++Glucose, Day 22, +Glucose, Day 22, +++Glucose, Day 29, TraceGlucose, Day 29, ++Glucose, Day 60, +Glucose, Day 60, ++Glucose, Day 90, +Glucose, Day 90, ++Glucose, Day 90, +++Glucose, Day 120, TraceGlucose, Day 120, +Glucose, Day 120, ++Glucose, Day 120, +++Glucose, Day 120, ++++Ketones, Day 1, TraceKetones, Day 1, +Ketones, Day1, ++Ketones, Day1, +++Ketones, Day 3, TraceKetones, Day 3, +Ketones, Day 3, ++Ketones, Day 3, +++Ketones, Day 5, +Ketones, Day 8, +Ketones, Day 11, TraceKetones, Day 22, TraceKetones, Day 22, +Ketones, Day 90, TraceKetones, Day 90, +Ketones, Day 90, ++Ketones, Day 120, TraceKetones, Day 120, +Ketones, Day 120, ++LE, Day 1, TraceLE, Day 1, +LE, Day1, ++LE, Day1, +++LE, Day 3, TraceLE, Day 3, +LE, Day 3, ++LE, Day 3, +++LE, Day 5, TraceLE, Day 5, +LE, Day 5, ++LE, Day 5, +++LE, Day 8, TraceLE, Day 8, +LE, Day 8, ++LE, Day 8, +++LE, Day 11, TraceLE, Day 11, +LE, Day 11, ++LE, Day 11, +++LE, Day 15, TraceLE, Day 15, +LE, Day 15, ++LE, Day 15, +++LE, Day 22, TraceLE, Day 22, +LE, Day 22, ++LE, Day 22, +++LE, Day 29, TraceLE, Day 29, +LE, Day 29, ++LE, Day 29, +++LE, Day 60, TraceLE, Day 60, +LE, Day 60, ++LE, Day 60, +++LE, Day 90, TraceLE, Day 90, +LE, Day 90, ++LE, Day 90, +++LE, Day 120, TraceLE, Day 120, +LE, Day 120, ++LE, Day 120, +++Nitrite, Day 1, TraceNitrite, Day 1, +Nitrite, Day 3, +Nitrite, Day 5, +Nitrite, Day 5, +++Nitrite, Day 8, +++Nitrite, Day 11, +Nitrite, Day 15, +Nitrite, Day 22, TraceNitrite, Day 29, +Nitrite, Day 60, +Nitrite, Day 90, TraceNitrite, Day 90, +Nitrite, Day 120, +Nitrite, Day 120, ++Occult blood, Day 1, TraceOccult blood, Day 1, +Occult blood, Day 1, ++Occult blood, Day1, +++Occult blood, Day1, ++++Occult blood, Day 3, TraceOccult blood, Day 3, +Occult blood, Day 3, ++Occult blood, Day 3, +++Occult blood, Day 3, ++++Occult blood, Day 5, TraceOccult blood, Day 5, +Occult blood, Day 5, ++Occult blood, Day 5, +++Occult blood, Day 5, ++++Occult blood, Day 8, TraceOccult blood, Day 8, +Occult blood, Day 8, ++Occult blood, Day 8,+++Occult blood, Day 11, TraceOccult blood, Day 11, +Occult blood, Day 11, ++Occult blood, Day 11, +++Occult blood, Day 11, ++++Occult blood, Day 15, TraceOccult blood, Day 15, +Occult blood, Day 15, ++Occult blood, Day 15, +++Occult blood, Day 15, ++++Occult blood, Day 22, TraceOccult blood, Day 22, +Occult blood, Day 22, ++Occult blood, Day 22, +++Occult blood, Day 22, ++++Occult blood, Day 29, TraceOccult blood, Day 29, +Occult blood, Day 29, ++Occult blood, Day 29, +++Occult blood, Day 29, ++++Occult blood, Day 60, TraceOccult blood, Day 60, +Occult blood, Day 60, ++Occult blood, Day 60, +++Occult blood, Day 60, ++++Occult blood, Day 90, TraceOccult blood, Day 90, +Occult blood, Day 90, ++Occult blood, Day 90, +++Occult blood, Day 90, ++++Occult blood, Day 120, TraceOccult blood, Day 120, +Occult blood, Day 120, ++Occult blood, Day 120, +++Occult blood, Day 120, ++++Protein, Day 1, TraceProtein, Day 1, +Protein, Day1, ++Protein, Day 3, TraceProtein, Day 3, +Protein, Day 3, ++Protein, Day 5, TraceProtein, Day 5, +Protein, Day 5, ++Protein, Day 8, TraceProtein, Day 8, +Protein, Day 8,++Protein, Day 11, TraceProtein, Day 11, +Protein, Day 11, ++Protein, Day 15, +Protein, Day 15, ++Protein, Day 22, TraceProtein, Day 22, +Protein, Day 22, ++Protein, Day 29, TraceProtein, Day 29, +Protein, Day 29, ++Protein, Day 60, TraceProtein, Day 60, +Protein, Day 60, ++Protein, Day 90, TraceProtein Day 90, +Protein, Day 120, TraceProtein, Day 120, +Protein, Day 120, ++Urobilinogen, Day 1, TraceUrobilinogen, Day 1, +Urobilinogen, Day1, ++Urobilinogen, Day1, +++Urobilinogen, Day 3, TraceUrobilinogen, Day 3, +Urobilinogen, Day 3, ++Urobilinogen Day 3, +++Urobilinogen, Day 3, ++++Urobilinogen, Day 5, TraceUrobilinogen, Day 5, +Urobilinogen, Day 8, TraceUrobilinogen, Day 8, +Urobilinogen, Day 8, ++Urobilinogen, Day 8,+++Urobilinogen, Day 11, TraceUrobilinogen, Day 11, +Urobilinogen, Day 11, ++Urobilinogen, Day 15, TraceUrobilinogen, Day 15, +Urobilinogen, Day 15, ++Urobilinogen, Day 22, TraceUrobilinogen, Day 29, TraceUrobilinogen, Day 29, +Urobilinogen, Day 60, TraceUrobilinogen, Day 60, +Urobilinogen, Day 90, TraceUrobilinogen, Day 90, +Urobilinogen, Day 120, TraceUrobilinogen, Day 120, +Urobilinogen, Day 120, ++
PQ+CQ12030002110111211311121131111201101210241111012200231132001010010000192205101422341223312831240106403421172113210000001000011104742136331133224402132011221115111251400730017232253028816131511420310001101001201010005412114311222111011000111010001
TQ+CQ1938214010102032020010000100003101010110100111001344205331111120111131951413213113371062611338442413315111488526132051250141111121230221218912641495347643412332833121132041142151733151523141374221336015194821354266114121221341331432618231036148003320001203113423143220

Number of Participants With Action Taken to Treat Relapse Episode of P. Vivax Malaria

Health outcomes were evaluated based on the actions taken by the participants to treat relapse episode of P vivax malaria. The number of participants with the type of action taken to treat relapse episode of P vivax malaria has been presented by country. Participants may be represented in more than one category, so the total number of participants may be less than the number quoted. Only those participants with data available at the specified data points were analyzed (represented by n=X in category title). (NCT02216123)
Timeframe: Up to Day 180

,
InterventionParticipants (Number)
Brazil; Trial clinic; n=19, 17Brazil; Other; n=19, 17Colombia; Nothing; n=4, 3Colombia; Trial clinic; n=4, 3Colombia; Another clinic; n=4, 3Colombia; Hospital emergency center; n=4, 3Peru; Trial clinic; n=33, 33Peru; Another clinic; n=33, 33Peru; Other; n=33, 33Thailand; Nothing; n=1, 1Thailand; Trial Clinic; n=1, 1Vietnam; Nothing; n=4, 7Vietnam; Drug Shop; n=4, 7Vietnam; Other; n=4, 7Vietnam; Another clinic; n=4, 7
First Malaria Relapse19521113289101210
First Malaria Relapse Follow-up170200133330015201

Number of Participants With Change in Best Corrected Visual Acuity Test Scores

Ophthalmic assessments were carried out at pre-qualified sites prior to randomization and at Days 29 and 90 and at withdrawal. Assessments were carried out at Day 180 if the Day 90 assessments showed abnormalities. The last assessment performed on the day of randomization or earlier was considered Baseline. Change from Baseline is the value at post dose visit minus the Baseline value. Best corrected visual acuity was assessed individually for each eye. Scores were recorded as a ratio. The values were used to derive a logMAR score for statistical analysis where logMAR=-1x log10 (ratio score). The number of participants with change in Best Corrected Visual Acuity Test Scores from Baseline has been presented where possible change is defined as a change from Baseline >=0.12 to <0.3 and definite change is defined as a change from Baseline >=0.3 logMAR score. Only those participants with data available at the specified data points were analyzed (represented by n=X in category title). (NCT02216123)
Timeframe: Baseline and up to Day 180

,
InterventionParticipants (Number)
Maximum change; possible; right eye; n=27, 13Maximum change; definite; right eye; n=27, 13Maximum change; possible; left eye; n=27, 13Maximum change; definite; left eye; n=27, 13Day 29; possible change; right eye; n=27, 13Day 29; definite change; right eye; n=27, 13Day 29; possible change; left eye; n=27, 13Day 29; definite change; left eye; n=27, 13Day 90; possible change; right eye; n=27, 12Day 90; definite change; right eye; n=27, 12Day 90; possible change; left eye; n=27, 12Day 90; definite change; left eye; n=27, 12Day 180; possible change; right eye; n=2, 2Day 180; definite change; right eye; n=2, 2Day 180; possible change; left eye; n=2, 2Day 180; definite change; left eye; n=2, 2
PQ+CQ0001000000000001
TQ+CQ1021102000210000

Number of Participants With Clinical Chemistry Laboratory Data Outside the Reference Range

Plasma or serum samples were anlalyzed to evaluate clinical chemistry parameters such as alanine aminotransferase (ALT), alkaline phosphatase (ALP), aspartate aminotransferase (AST), bilirubin, creatine kinase, creatinine, glomerular filtration rate (GFR), indirect bilirubin and urea. The number of participants with clinical chemistry laboratory values outside the extended normal range (F3) has been presented. The upper and lower limits for F3 range were defined by multiplying the normal range limits by different factors. High and low indicated that the participants had values flagged as high and low respectively for the particular parameter any time on-treatment. Safety Population consisted of all randomized participants who received at least one dose of blinded study medication. (NCT02216123)
Timeframe: Up to Day 120

,
InterventionParticipants (Number)
ALT, HighALP, HighAST, HighBilirubin, HighCreatine kinase, HighCreatinine, HighGFR, LowIndirect bilirubin, HighUrea, High
PQ+CQ013184002119
TQ+CQ806283003640

Number of Participants With Electrocardiogram (ECG) Findings

12 lead ECG was performed with the participant in a semi-supine position having rested in this position for at least 10 minutes. ECG assessments were performed in triplicate at screening followed by single ECGs 12 hours after the first dose of study medication and at Day 29. The number of participants with abnormal-clinically significant ECG findings have been presented. The 12 Hour Post Randomized Treatment (11.5-12.5 Hours) timepoint included all readings taken between 11.5 and 12.5 hours post randomized treatment. The 12 Hour Post Randomized Treatment (8-72 Hours) timepoint is a sensitivity analysis of the 12 Hour post randomized treatment timepoint, including all readings taken between 8 and 72 hours post randomized treatment. Only those participants with data available at the specified data points were analyzed (represented by n=X in category title). (NCT02216123)
Timeframe: Up to Day 29

,
InterventionParticipants (Number)
11.5 to 12.5 hours Day 1, Assessment 1; n=143, 7511.5 to 12.5 hours Day 1 Assessment 2; n=6, 611.5 to 12.5 hours Day 1 Assessment 3; n=5, 58 to 72 hours Day 1 Assessment 1; n=166, 858 to 72 hours Day 1 Assessment 2; n=6, 68 to 72 hours Day 1 Assessment 3; n=5, 5Day 29; n=161, 84
PQ+CQ0000000
TQ+CQ0000000

Number of Participants With Genetically Homologous and Genetically Heterologous P. Vivax Infections

Two drops of peripheral blood were collected onto pre-printed filter paper for subsequent deoxyribonucleic acid (DNA) extraction and polymerase chain reaction (PCR) analysis of Plasmodium species on all participants at screening (Day 1; pre-dose) and; if necessary, at the time of the first recrudescence/relapse or re-infection. PCR of the P. vivax genes, was used to distinguish between genetically homologous and genetically heterologous infection. The number of participants with genetically homologous and genetically heterologous P. vivax infections has been summarized for each treatment group. Only those participants with an infection occuring on or after Study Day 33 were analyzed. (NCT02216123)
Timeframe: Up to Day 180

,
InterventionParticipants (Number)
Heterologous P. vivaxHomologous P. vivaxUnknown genetic classification
PQ+CQ9101
TQ+CQ8295

Number of Participants With Hematology Laboratory Data Outside the Reference Range

Blood samples were collected for the evaluation of hematology parameters including eosinophils, leukocytes, lymphocytes, neutrophils, platelets, reticulocytes and methemoglobin. The number of participants with hematology laboratory data outside the extended normal range (F3) has been presented. The upper and lower limits for F3 range were defined by multiplying the normal range limits by different factors. High and low indicated that the participants had values flagged as high and low respectively for the particular parameter any time on-treatment. Participants having both High and Low values for Normal Ranges at any post-baseline visits for safety parameters were counted in both the High and Low categories. (NCT02216123)
Timeframe: Up to Day 120

,
InterventionParticipants (Number)
Blood eosinophils, HighBlood leukocytes, LowBlood lymphocytes, LowBlood lymphocytes, HighBlood neutrophils, LowBlood platelets, LowBlood reticulocytes, HighMethemoglobin, High
PQ+CQ1501438393
TQ+CQ320811513802

Number of Participants With Keratopathy

Ophthalmic assessments were carried out at pre-qualified sites prior to randomization and at Days 29 and 90 and at withdrawal follow-up visit. Assessments were carried out at Day 180 (and up to resolution) if the Day 90 assessments showed abnormalities. The last assessment performed on the day of randomization or earlier was considered Baseline. The number of participants displaying keratopathy in each eye has been summarized for each visit. The number of participants with new keratopathy at any time post Baseline is also reported. Ophthalmic Safety Population comprised of all participants in the Safety Population who have results from any eye assessments. Only those participants with data available at the specified data points were analyzed (represented by n=X in category title). (NCT02216123)
Timeframe: Up to Day 180

,
InterventionParticipants (Number)
Baseline; right eye; n=27, 13Baseline; left eye; n=27, 13Day 1; right eye; n=27, 13Day 1; left eye; n=27, 13Day 29; right eye; n=27, 13Day 29; left eye; n=27, 13Day 90; right eye; n=27, 12Day 90; left eye; n=27, 12Day 180; right eye; n=2, 2Day 180; left eye; n=2, 2Any time post Baseline; right eye; n=27, 13Any time post Baseline; left eye; n=27, 13
PQ+CQ000000000000
TQ+CQ000000000000

Number of Participants With Retinal Changes From Baseline

Ophthalmic assessments were carried out at pre-qualified sites prior to randomization and at Days 29 and 90 and at withdrawal follow-up. Assessments were carried out at Day 180 (and up to resolution) if the Day 90 assessments showed abnormalities. The last assessment performed on the day of randomization or earlier was considered Baseline. Change from Baseline was calculated as the value at post dose visit minus the Baseline value. The number of participants with definite retinal change and questionable (ques) retinal change from Baseline has been presented. The number of participants with maximum change post-Baseline (definite when absent or questionable at Baseline) has been presented for either eye. Only those participants with data available at the specified data points were analyzed (represented by n=X in category title). (NCT02216123)
Timeframe: Baseline and up to Day 180

,
InterventionParticipants (Number)
Day 29, Definite change, right eye; n=22, 13Day 29, Ques change, right eye; n=22, 13Day 29, Definite change, left eye; n=22, 13Day 29, Ques change, left eye; n=22, 13Day 90, Definite change, right eye; n=24, 11Day 90, Ques change, right eye; n=24, 11Day 90, Definite change, left eye; n=24, 11Day 90, Ques change, left eye; n=24, 11Day 180, Definite change, right eye; n=3, 2Day 180, Ques change, right eye; n=3, 2Day 180, Definite change, left eye; n=3, 2Day 180, Ques change, left eye; n=3, 2Maximum change post-Baseline; either eye; n=27, 13
PQ+CQ0000010000000
TQ+CQ0201020000000

Number of Participants With Treatment Emergent Adverse Events (TEAEs) and Serious TEAEs

An adverse event (AE) is defined as any untoward medical occurrence in a participant under clinical investigation, temporally associated with the use of a medicinal product, whether or not considered related to the medicinal product. Serious adverse event (SAE) is defined as any untoward medical occurrence that, at any dose results in death, is life-threatening, requires hospitalization or prolongation of existing hospitalization, results in disability/incapacity, is a congenital anomaly/ birth defect, other situations such as important medical events and events of possible drug induced liver injury with hyperbilirubinemia. TEAEs are defined as AEs with an onset date and time on or after that of the start of first dose of study medication (including CQ). Number of participants with TEAEs and serious TEAEs have been presented. (NCT02216123)
Timeframe: Up to Day 180

,
InterventionParticipants (Number)
TEAEsSerious TEAEs
PQ+CQ641
TQ+CQ1196

Time to Parasitemia for Immunogenicity Population

"Subjects were ranked according to time of onset of parasitemia and a non-parametric rankorder statistical test (eg, Log-Rank or Mann-Whitney) was performed to evaluate delays in parasitemia induced by vaccination. Cox Proportional Hazards model was used to calculate days to parasitemia and Kaplan-Meier plots were used to display time to first positive malaria blood smear.~Hazard Ratio (HR). Time starts once subject has received t infectious bites. Time stops when subject has first positive blood smear. If subject does not become parasitemic then time stops the day he/she begins anti-malarial therapy." (NCT01157897)
Timeframe: 280 day (during the study through 6 months aftr challenge)

Interventiondays (Mean)
Cohort 1: 15 μg VMP0010.137
Cohort 2: 30 μg VMP0010.073
Cohort 3: 60 μg VMP0010.042

Geometric Mean of Anti-VMP001 Anti-body Titers in Serum Per Efficacy Population

Anti-VMP001 antibody concentrations were measured and summarized by geometric mean titers (GMT) with 95% confidence interval (CI). Peak responses were compared by performing Student's t-test on data normalized by log transformation to ascertain the presence or absence of significant dose response differences. ELISA Units (EU) were converted to log10 values for calculations and statistical comparison of geometric means. Units that were reported as '>50' were converted to '1'. (NCT01157897)
Timeframe: study duration

,,
InterventionGeometric Mean Titier of European Units (Mean)
Pre-vaccination2wks post first vaccinationDay of second vaccination2wks post second vaccinationDay of third vaccination2wks post third vaccination4wks post challenge6mths post challenge
Cohort 1: 15 μg VMP0011133.72244.3520161.189053.3261203.4854843.3810860.7
Cohort 2: 30 μg VMP0011750.381450.2281143.7231071.0168730.456472.1712519.16
Cohort 3: 60 μg VMP0013.09836.681711.6361711.836405.6641879.9932178.395500.73

Geometric Mean of Anti-VMP001 Antibody Titers in Serum Per Immunogenicity Population

Anti-VMP001 antibody concentrations were measured and summarized by geometric mean titers (GMT) with 95% confidence interval (CI). Peak responses were compared by performing Student's t-test on data normalized by log transformation to ascertain the presence or absence of significant dose response differences. ELISA Units (EU) were converted to log10 values for calculations and statistical comparison of geometric means. Units that were reported as '>50' were converted to '1'. (NCT01157897)
Timeframe: study duration

,,
InterventionGeometric Mean Titer of European Units (Mean)
Pre-vaccination2wks post first vaccinationDay of second vaccination2wks post second vaccinationDay of third vaccination2wks post third vaccination4wks post challenge6months post challenge
Cohort 1: 15 μg VMP0011151.39281.7921862.229921.6159883.7754843.3810860.7
Cohort 2: 30 μg VMP0011.5526.181175.4174608.6228498.4368730.456472.1712519.16
Cohort 3: 60 μg VMP0013.09836.681711.6361711.836405.6641879.9932178.395500.73

Occurrence of Solicited Adverse Events Over a 7 Day Follow-up Period After Each Immunization (the Day of the Immunization and 6 Subsequent Days) During the Vaccination Phase

Adverse events were evaluated for 7 days after each vaccination during the vaccine phase. (NCT01157897)
Timeframe: 7 days after immunization

,,
Interventionparticipants with AEs (Number)
Solicited Local: Injection site erythemaSolicited Local: Injection site indurationSolicited Local: Injection site painSolicited Systemic: DiarrheaSolicited Systemic: NauseaSolicited Systemic: VomitingSolicited Systemic: FatigueSolicited Systemic: PyrexiaSolicited Systemic: ArthralgiaSolicited Systemic: MyalgiaSolicited Systemic: Headache
Cohort 1: 15 μg VMP001201005284448
Cohort 2: 30 μg VMP001311003042246
Cohort 3: 60 μg VMP001621014271375

Occurrence of Unsolicited Adverse Events Over a 28 Day Follow-up Period After Each Immunization (the Day of the Immunization and 27 Subsequent Days) During the Vaccination Phase

Adverse events were evaluated over a 28 day follow-up period after each vaccination during the vaccine phase (NCT01157897)
Timeframe: 28 days following immunization

,,
Interventionparticipants with AEs (Number)
Ear discomfortAbdominal discomfortAbdominal painFeces discoloredFood poisoningNauseaToothacheAxillary painChillsFeeling hotInjection site erythemaInjection site pruritusInjection site swellingInjection site warmthMalaiseHypertransaminasaemiaSeasonal allergyNasopharyngitisUpper respiratory tract infectionContusionExcoriationPostprocedural discomfortPosttraumatic painScratchSkin lacerationHaemoglobin decreasedPlatelet count decreasedGoutBack painMuscle spasmsMusculoskeletal discomfortMyalgiaPain in extremityDizzinessHeadacheSinus headacheNasal CongestionCold sweatDermatitis contactErythemaHypertension
Cohort 1: 15 μg VMP00111001120550000311120000000010111211002001
Cohort 2: 30 μg VMP00100000001560021520000010001101000000004110
Cohort 3: 60 μg VMP00100110000771132711021101121101010210112000

Infection for P. Vivax

Thick blood smear was performed to patients daily on days 7 to 23, and every other day until day 29. Any prove of P. vivax infection was considered positive and confirmed later by real time polymerase chain reaction (rPCR). (NCT00367380)
Timeframe: Twenty eight days

Interventiondays (Mean)
Group 111
Group 211
Group 39

Reviews

4 reviews available for primaquine and Parasitemia

ArticleYear
Tafenoquine for preventing relapse in people with Plasmodium vivax malaria.
    The Cochrane database of systematic reviews, 2020, 09-06, Volume: 9

    Topics: Adult; Aminoquinolines; Antimalarials; Chloroquine; Drug Administration Schedule; Glucosephosphate D

2020
Artemisinin-based combination therapy for treating uncomplicated Plasmodium vivax malaria.
    The Cochrane database of systematic reviews, 2013, Oct-25, Issue:10

    Topics: Antimalarials; Artemether, Lumefantrine Drug Combination; Artemisinins; Drug Combinations; Drug Resi

2013
Clinical implications of a gradual dormancy concept in malaria.
    Parasitology research, 2016, Volume: 115, Issue:6

    Topics: Aminoquinolines; Antimalarials; Humans; Liver; Malaria; Parasitemia; Plasmodium; Plasmodium falcipar

2016
Rationale for recommending a lower dose of primaquine as a Plasmodium falciparum gametocytocide in populations where G6PD deficiency is common.
    Malaria journal, 2012, Dec-14, Volume: 11

    Topics: Adult; Anemia, Hemolytic; Animals; Anopheles; Antimalarials; Artemisinins; Drug Therapy, Combination

2012

Trials

34 trials available for primaquine and Parasitemia

ArticleYear
Ultra-short course, high-dose primaquine to prevent Plasmodium vivax infection following uncomplicated pediatric malaria: A randomized, open-label, non-inferiority trial of early versus delayed treatment.
    International journal of infectious diseases : IJID : official publication of the International Society for Infectious Diseases, 2023, Volume: 130

    Topics: Antimalarials; Artemether; Artemether, Lumefantrine Drug Combination; Child; Humans; Malaria; Malari

2023
Primaquine radical cure in patients with Plasmodium falciparum malaria in areas co-endemic for P falciparum and Plasmodium vivax (PRIMA): a multicentre, open-label, superiority randomised controlled trial.
    Lancet (London, England), 2023, Dec-02, Volume: 402, Issue:10417

    Topics: Antimalarials; Artemether; Artemether, Lumefantrine Drug Combination; Australia; Humans; Malaria; Ma

2023
Parasite clearance, cure rate, post-treatment prophylaxis and safety of standard 3-day versus an extended 6-day treatment of artemether-lumefantrine and a single low-dose primaquine for uncomplicated Plasmodium falciparum malaria in Bagamoyo district, Tan
    Malaria journal, 2020, Jun-23, Volume: 19, Issue:1

    Topics: Adolescent; Adult; Antimalarials; Artemether, Lumefantrine Drug Combination; Child; Child, Preschool

2020
Safety and Efficacy of Adding a Single Low Dose of Primaquine to the Treatment of Adult Patients With Plasmodium falciparum Malaria in Senegal, to Reduce Gametocyte Carriage: A Randomized Controlled Trial.
    Clinical infectious diseases : an official publication of the Infectious Diseases Society of America, 2017, 08-15, Volume: 65, Issue:4

    Topics: Adolescent; Adult; Aged; Antimalarials; Female; Hemoglobins; Humans; Malaria, Falciparum; Male; Midd

2017
Comparison of the Cumulative Efficacy and Safety of Chloroquine, Artesunate, and Chloroquine-Primaquine in Plasmodium vivax Malaria.
    Clinical infectious diseases : an official publication of the Infectious Diseases Society of America, 2018, 10-30, Volume: 67, Issue:10

    Topics: Adolescent; Adult; Antimalarials; Artesunate; Child; Child, Preschool; Chloroquine; Drug Therapy, Co

2018
Comparison of the Cumulative Efficacy and Safety of Chloroquine, Artesunate, and Chloroquine-Primaquine in Plasmodium vivax Malaria.
    Clinical infectious diseases : an official publication of the Infectious Diseases Society of America, 2018, 10-30, Volume: 67, Issue:10

    Topics: Adolescent; Adult; Antimalarials; Artesunate; Child; Child, Preschool; Chloroquine; Drug Therapy, Co

2018
Comparison of the Cumulative Efficacy and Safety of Chloroquine, Artesunate, and Chloroquine-Primaquine in Plasmodium vivax Malaria.
    Clinical infectious diseases : an official publication of the Infectious Diseases Society of America, 2018, 10-30, Volume: 67, Issue:10

    Topics: Adolescent; Adult; Antimalarials; Artesunate; Child; Child, Preschool; Chloroquine; Drug Therapy, Co

2018
Comparison of the Cumulative Efficacy and Safety of Chloroquine, Artesunate, and Chloroquine-Primaquine in Plasmodium vivax Malaria.
    Clinical infectious diseases : an official publication of the Infectious Diseases Society of America, 2018, 10-30, Volume: 67, Issue:10

    Topics: Adolescent; Adult; Antimalarials; Artesunate; Child; Child, Preschool; Chloroquine; Drug Therapy, Co

2018
Single-Dose Tafenoquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Cytochrome P-450 CYP2D6; Disease-Fre

2019
Single-Dose Tafenoquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Cytochrome P-450 CYP2D6; Disease-Fre

2019
Single-Dose Tafenoquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Cytochrome P-450 CYP2D6; Disease-Fre

2019
Single-Dose Tafenoquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Cytochrome P-450 CYP2D6; Disease-Fre

2019
Single-Dose Tafenoquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Cytochrome P-450 CYP2D6; Disease-Fre

2019
Single-Dose Tafenoquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Cytochrome P-450 CYP2D6; Disease-Fre

2019
Single-Dose Tafenoquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Cytochrome P-450 CYP2D6; Disease-Fre

2019
Single-Dose Tafenoquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Cytochrome P-450 CYP2D6; Disease-Fre

2019
Single-Dose Tafenoquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Cytochrome P-450 CYP2D6; Disease-Fre

2019
Tafenoquine versus Primaquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Disease-Free Survival; Double-Blind

2019
Tafenoquine versus Primaquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Disease-Free Survival; Double-Blind

2019
Tafenoquine versus Primaquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Disease-Free Survival; Double-Blind

2019
Tafenoquine versus Primaquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Disease-Free Survival; Double-Blind

2019
Tafenoquine versus Primaquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Disease-Free Survival; Double-Blind

2019
Tafenoquine versus Primaquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Disease-Free Survival; Double-Blind

2019
Tafenoquine versus Primaquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Disease-Free Survival; Double-Blind

2019
Tafenoquine versus Primaquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Disease-Free Survival; Double-Blind

2019
Tafenoquine versus Primaquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Disease-Free Survival; Double-Blind

2019
Tafenoquine versus Primaquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Disease-Free Survival; Double-Blind

2019
Tafenoquine versus Primaquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Disease-Free Survival; Double-Blind

2019
Tafenoquine versus Primaquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Disease-Free Survival; Double-Blind

2019
Tafenoquine versus Primaquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Disease-Free Survival; Double-Blind

2019
Tafenoquine versus Primaquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Disease-Free Survival; Double-Blind

2019
Tafenoquine versus Primaquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Disease-Free Survival; Double-Blind

2019
Tafenoquine versus Primaquine to Prevent Relapse of Plasmodium vivax Malaria.
    The New England journal of medicine, 2019, 01-17, Volume: 380, Issue:3

    Topics: Adolescent; Adult; Aminoquinolines; Antimalarials; Chloroquine; Disease-Free Survival; Double-Blind

2019
The tolerability of single low dose primaquine in glucose-6-phosphate deficient and normal falciparum-infected Cambodians.
    BMC infectious diseases, 2019, Mar-12, Volume: 19, Issue:1

    Topics: Adolescent; Adult; Aged; Antimalarials; Artemisinins; Cambodia; Child; Child, Preschool; Female; Glu

2019
Short-course primaquine for the radical cure of Plasmodium vivax malaria: a multicentre, randomised, placebo-controlled non-inferiority trial.
    Lancet (London, England), 2019, 09-14, Volume: 394, Issue:10202

    Topics: Adolescent; Adult; Antimalarials; Child; Child, Preschool; Double-Blind Method; Drug Administration

2019
Nonrandomized controlled trial of artesunate plus sulfadoxine-pyrimethamine with or without primaquine for preventing posttreatment circulation of Plasmodium falciparum gametocytes.
    Antimicrobial agents and chemotherapy, 2013, Volume: 57, Issue:7

    Topics: Adolescent; Adult; Antimalarials; Artemisinins; Child; Child, Preschool; Drug Combinations; Drug The

2013
In vivo efficacy of artemether-lumefantrine and chloroquine against Plasmodium vivax: a randomized open label trial in central Ethiopia.
    PloS one, 2013, Volume: 8, Issue:5

    Topics: Adolescent; Adult; Aged; Antimalarials; Artemether; Artemisinins; Child; Child, Preschool; Chloroqui

2013
Primaquine failure and cytochrome P-450 2D6 in Plasmodium vivax malaria.
    The New England journal of medicine, 2013, Oct-03, Volume: 369, Issue:14

    Topics: Adolescent; Adult; Cytochrome P-450 CYP2D6; Female; Humans; Malaria, Vivax; Male; Metabolism, Inborn

2013
Primaquine failure and cytochrome P-450 2D6 in Plasmodium vivax malaria.
    The New England journal of medicine, 2013, Oct-03, Volume: 369, Issue:14

    Topics: Adolescent; Adult; Cytochrome P-450 CYP2D6; Female; Humans; Malaria, Vivax; Male; Metabolism, Inborn

2013
Primaquine failure and cytochrome P-450 2D6 in Plasmodium vivax malaria.
    The New England journal of medicine, 2013, Oct-03, Volume: 369, Issue:14

    Topics: Adolescent; Adult; Cytochrome P-450 CYP2D6; Female; Humans; Malaria, Vivax; Male; Metabolism, Inborn

2013
Primaquine failure and cytochrome P-450 2D6 in Plasmodium vivax malaria.
    The New England journal of medicine, 2013, Oct-03, Volume: 369, Issue:14

    Topics: Adolescent; Adult; Cytochrome P-450 CYP2D6; Female; Humans; Malaria, Vivax; Male; Metabolism, Inborn

2013
Primaquine failure and cytochrome P-450 2D6 in Plasmodium vivax malaria.
    The New England journal of medicine, 2013, Oct-03, Volume: 369, Issue:14

    Topics: Adolescent; Adult; Cytochrome P-450 CYP2D6; Female; Humans; Malaria, Vivax; Male; Metabolism, Inborn

2013
Primaquine failure and cytochrome P-450 2D6 in Plasmodium vivax malaria.
    The New England journal of medicine, 2013, Oct-03, Volume: 369, Issue:14

    Topics: Adolescent; Adult; Cytochrome P-450 CYP2D6; Female; Humans; Malaria, Vivax; Male; Metabolism, Inborn

2013
Primaquine failure and cytochrome P-450 2D6 in Plasmodium vivax malaria.
    The New England journal of medicine, 2013, Oct-03, Volume: 369, Issue:14

    Topics: Adolescent; Adult; Cytochrome P-450 CYP2D6; Female; Humans; Malaria, Vivax; Male; Metabolism, Inborn

2013
Primaquine failure and cytochrome P-450 2D6 in Plasmodium vivax malaria.
    The New England journal of medicine, 2013, Oct-03, Volume: 369, Issue:14

    Topics: Adolescent; Adult; Cytochrome P-450 CYP2D6; Female; Humans; Malaria, Vivax; Male; Metabolism, Inborn

2013
Primaquine failure and cytochrome P-450 2D6 in Plasmodium vivax malaria.
    The New England journal of medicine, 2013, Oct-03, Volume: 369, Issue:14

    Topics: Adolescent; Adult; Cytochrome P-450 CYP2D6; Female; Humans; Malaria, Vivax; Male; Metabolism, Inborn

2013
The efficacy of artesunate, chloroquine, doxycycline, primaquine and a combination of artesunate and primaquine against avian malaria in broilers.
    The Journal of veterinary medical science, 2014, Volume: 76, Issue:6

    Topics: Analysis of Variance; Animals; Antimalarials; Artemisinins; Artesunate; Body Weight; Chickens; Chlor

2014
Adding a single low-dose of primaquine (0.25 mg/kg) to artemether-lumefantrine did not compromise treatment outcome of uncomplicated Plasmodium falciparum malaria in Tanzania: a randomized, single-blinded clinical trial.
    Malaria journal, 2016, Aug-26, Volume: 15, Issue:1

    Topics: Adolescent; Antimalarials; Artemether, Lumefantrine Drug Combination; Artemisinins; Child; Child, Pr

2016
Therapeutic efficacy of chloroquine and chloroquine plus primaquine for the treatment of Plasmodium vivax in Ethiopia.
    Acta tropica, 2010, Volume: 113, Issue:2

    Topics: Adolescent; Adult; Aged; Antimalarials; Child; Child, Preschool; Chloroquine; Drug Resistance; Drug

2010
[Therapeutic efficacy of a regimen of artesunate-mefloquine-primaquine treatment for Plasmodium falciparum malaria and treatment effects on gametocytic development].
    Biomedica : revista del Instituto Nacional de Salud, 2009, Volume: 29, Issue:2

    Topics: Adolescent; Adult; Animals; Antimalarials; Artemisinins; Artesunate; Child; Drug Resistance; Drug Th

2009
Clinical and parasitological response to oral chloroquine and primaquine in uncomplicated human Plasmodium knowlesi infections.
    Malaria journal, 2010, Aug-19, Volume: 9

    Topics: Administration, Oral; Adult; Antimalarials; Borneo; Chloroquine; Drug Therapy, Combination; Female;

2010
Consistent safety and infectivity in sporozoite challenge model of Plasmodium vivax in malaria-naive human volunteers.
    The American journal of tropical medicine and hygiene, 2011, Volume: 84, Issue:2 Suppl

    Topics: Adult; Animals; Antimalarials; Chloroquine; Duffy Blood-Group System; Female; Fever; Humans; Malaria

2011
Consistent safety and infectivity in sporozoite challenge model of Plasmodium vivax in malaria-naive human volunteers.
    The American journal of tropical medicine and hygiene, 2011, Volume: 84, Issue:2 Suppl

    Topics: Adult; Animals; Antimalarials; Chloroquine; Duffy Blood-Group System; Female; Fever; Humans; Malaria

2011
Consistent safety and infectivity in sporozoite challenge model of Plasmodium vivax in malaria-naive human volunteers.
    The American journal of tropical medicine and hygiene, 2011, Volume: 84, Issue:2 Suppl

    Topics: Adult; Animals; Antimalarials; Chloroquine; Duffy Blood-Group System; Female; Fever; Humans; Malaria

2011
Consistent safety and infectivity in sporozoite challenge model of Plasmodium vivax in malaria-naive human volunteers.
    The American journal of tropical medicine and hygiene, 2011, Volume: 84, Issue:2 Suppl

    Topics: Adult; Animals; Antimalarials; Chloroquine; Duffy Blood-Group System; Female; Fever; Humans; Malaria

2011
A cluster-randomized trial of mass drug administration with a gametocytocidal drug combination to interrupt malaria transmission in a low endemic area in Tanzania.
    Malaria journal, 2011, Aug-24, Volume: 10

    Topics: Adolescent; Adult; Aged; Aged, 80 and over; Antimalarials; Artemisinins; Artesunate; Child; Child, P

2011
A cluster-randomized trial of mass drug administration with a gametocytocidal drug combination to interrupt malaria transmission in a low endemic area in Tanzania.
    Malaria journal, 2011, Aug-24, Volume: 10

    Topics: Adolescent; Adult; Aged; Aged, 80 and over; Antimalarials; Artemisinins; Artesunate; Child; Child, P

2011
A cluster-randomized trial of mass drug administration with a gametocytocidal drug combination to interrupt malaria transmission in a low endemic area in Tanzania.
    Malaria journal, 2011, Aug-24, Volume: 10

    Topics: Adolescent; Adult; Aged; Aged, 80 and over; Antimalarials; Artemisinins; Artesunate; Child; Child, P

2011
A cluster-randomized trial of mass drug administration with a gametocytocidal drug combination to interrupt malaria transmission in a low endemic area in Tanzania.
    Malaria journal, 2011, Aug-24, Volume: 10

    Topics: Adolescent; Adult; Aged; Aged, 80 and over; Antimalarials; Artemisinins; Artesunate; Child; Child, P

2011
Efficacy of different primaquine-based antimalarial regimens against Plasmodium falciparum gametocytemia.
    Acta tropica, 2012, Volume: 122, Issue:2

    Topics: Adolescent; Adult; Aged; Amodiaquine; Antimalarials; Artemisinins; Artesunate; Child; Child, Prescho

2012
Short report: therapeutic efficacy of chloroquine combined with primaquine against Plasmodium falciparum in northeastern Papua, Indonesia.
    The American journal of tropical medicine and hygiene, 2002, Volume: 66, Issue:6

    Topics: Antimalarials; Chloroquine; Drug Therapy, Combination; Humans; Incidence; Indonesia; Malaria, Falcip

2002
The efficacy of combined mefloquine-artesunate versus mefloquine-primaquine on subsequent development of Plasmodium falciparum gametocytemia.
    The American journal of tropical medicine and hygiene, 2003, Volume: 68, Issue:5

    Topics: Adolescent; Adult; Animals; Antimalarials; Artemisinins; Artesunate; Carrier State; Child; Drug Resi

2003
CV8, a new combination of dihydroartemisinin, piperaquine, trimethoprim and primaquine, compared with atovaquone-proguanil against falciparum malaria in Vietnam.
    Tropical medicine & international health : TM & IH, 2004, Volume: 9, Issue:2

    Topics: Adolescent; Adult; Aged; Animals; Antimalarials; Artemisinins; Atovaquone; Drug Combinations; Drug T

2004
A prospective study evaluating the efficacy of a single, 45-mg dose of primaquine, as a gametocytocidal agent, in patients with Plasmodium falciparum malaria in Mumbai, India.
    Annals of tropical medicine and parasitology, 2004, Volume: 98, Issue:5

    Topics: Adolescent; Adult; Aged; Antimalarials; Chloroquine; Drug Administration Schedule; Drug Therapy, Com

2004
Preliminary report of the evaluation of the gametocytocidal action of bulaquine, in adult patients with acute, Plasmodium falciparum malaria.
    Annals of tropical medicine and parasitology, 2004, Volume: 98, Issue:5

    Topics: Acute Disease; Adult; Animals; Antimalarials; Drug Therapy, Combination; Humans; Malaria, Falciparum

2004
A double-blind, randomized study of azithromycin compared to chloroquine for the treatment of Plasmodium vivax malaria in India.
    The American journal of tropical medicine and hygiene, 2005, Volume: 73, Issue:6

    Topics: Adult; Aged; Animals; Antimalarials; Azithromycin; Chloroquine; Double-Blind Method; Drug Administra

2005
A randomized, parallel study of the safety and efficacy of 45 mg primaquine versus 75 mg bulaquine as gametocytocidal agents in adults with blood schizonticide-responsive uncomplicated falciparum malaria [ISCRTN50134587].
    BMC infectious diseases, 2006, Feb-01, Volume: 6

    Topics: Adolescent; Adult; Aged; Animals; Antimalarials; Doxycycline; Drug Administration Schedule; Drug The

2006
Efficacy of three chloroquine-primaquine regimens for treatment of Plasmodium vivax malaria in Colombia.
    The American journal of tropical medicine and hygiene, 2006, Volume: 75, Issue:4

    Topics: Adult; Animals; Antimalarials; Chloroquine; Colombia; Female; Follow-Up Studies; Humans; Malaria, Vi

2006
Clinical efficacy of chloroquine versus artemether-lumefantrine for Plasmodium vivax treatment in Thailand.
    The Korean journal of parasitology, 2007, Volume: 45, Issue:2

    Topics: Adolescent; Aged; Animals; Antimalarials; Artemether; Artemisinins; Chloroquine; Drug Therapy, Combi

2007
Primaquine for prophylaxis against malaria among nonimmune transmigrants in Irian Jaya, Indonesia.
    The American journal of tropical medicine and hygiene, 1995, Volume: 52, Issue:6

    Topics: Adolescent; Adult; Animals; Anopheles; Child; Chloroquine; Confounding Factors, Epidemiologic; Drug

1995
Malaria in a nonimmune population after extended chloroquine or primaquine prophylaxis.
    The American journal of tropical medicine and hygiene, 1997, Volume: 56, Issue:2

    Topics: Antimalarials; Chloroquine; Disease Susceptibility; Follow-Up Studies; Humans; Incidence; Indonesia;

1997
Halofantrine and primaquine for radical cure of malaria in Irian Jaya, Indonesia.
    Annals of tropical medicine and parasitology, 1997, Volume: 91, Issue:1

    Topics: Adult; Antimalarials; Chloroquine; Drug Therapy, Combination; Follow-Up Studies; Humans; Indonesia;

1997
Efficacy of primaquine regimens for primaquine-resistant Plasmodium vivax malaria in Thailand.
    The American journal of tropical medicine and hygiene, 1999, Volume: 61, Issue:6

    Topics: Adolescent; Adult; Aged; Animals; Antimalarials; Artemisinins; Artesunate; Drug Combinations; Drug R

1999
Plasmodium vivax clinically resistant to chloroquine in Colombia.
    The American journal of tropical medicine and hygiene, 2001, Volume: 65, Issue:2

    Topics: Animals; Antimalarials; Chloroquine; Colombia; Drug Therapy, Combination; Humans; Malaria, Vivax; Ma

2001
Plasmodium vivax clinically resistant to chloroquine in Colombia.
    The American journal of tropical medicine and hygiene, 2001, Volume: 65, Issue:2

    Topics: Animals; Antimalarials; Chloroquine; Colombia; Drug Therapy, Combination; Humans; Malaria, Vivax; Ma

2001
Plasmodium vivax clinically resistant to chloroquine in Colombia.
    The American journal of tropical medicine and hygiene, 2001, Volume: 65, Issue:2

    Topics: Animals; Antimalarials; Chloroquine; Colombia; Drug Therapy, Combination; Humans; Malaria, Vivax; Ma

2001
Plasmodium vivax clinically resistant to chloroquine in Colombia.
    The American journal of tropical medicine and hygiene, 2001, Volume: 65, Issue:2

    Topics: Animals; Antimalarials; Chloroquine; Colombia; Drug Therapy, Combination; Humans; Malaria, Vivax; Ma

2001

Other Studies

42 other studies available for primaquine and Parasitemia

ArticleYear
Discovery of new thienopyrimidinone derivatives displaying antimalarial properties toward both erythrocytic and hepatic stages of Plasmodium.
    European journal of medicinal chemistry, 2015, May-05, Volume: 95

    Topics: Animals; Antimalarials; Cell Proliferation; CHO Cells; Cricetinae; Cricetulus; Drug Discovery; Eryth

2015
Structure-activity relationship of new antimalarial 1-aryl-3-susbtituted propanol derivatives: Synthesis, preliminary toxicity profiling, parasite life cycle stage studies, target exploration, and targeted delivery.
    European journal of medicinal chemistry, 2018, May-25, Volume: 152

    Topics: Animals; Antimalarials; Cell Survival; Dose-Response Relationship, Drug; Drug Delivery Systems; Hep

2018
Blood-stage antiplasmodial activity and oocyst formation-blockage of metallo copper-cinchonine complex.
    Frontiers in cellular and infection microbiology, 2022, Volume: 12

    Topics: Animals; Antimalarials; Chloroquine; Copper; Malaria, Falciparum; Malaria, Vivax; Mice; Oocysts; Par

2022
Treatment of uncomplicated Plasmodium vivax with chloroquine plus radical cure with primaquine without G6PDd testing is safe in Arba Minch, Ethiopia: assessment of clinical and parasitological response.
    Malaria journal, 2023, Apr-25, Volume: 22, Issue:1

    Topics: Antimalarials; Chloroquine; Ethiopia; Humans; Malaria, Vivax; Parasitemia; Plasmodium vivax; Primaqu

2023
Liver Enzyme Elevations in
    The American journal of tropical medicine and hygiene, 2020, Volume: 103, Issue:1

    Topics: Acrylamides; Adamantane; Adult; Alanine Transaminase; Aminopyridines; Aminoquinolines; Antimalarials

2020
Case report of Plasmodium ovale curtisi malaria in Sri Lanka: relevance for the maintenance of elimination status.
    BMC infectious diseases, 2017, 04-24, Volume: 17, Issue:1

    Topics: Adult; Antimalarials; Chloroquine; Fever; Humans; Liberia; Malaria; Malaria, Vivax; Male; Molecular

2017
SLCO1A2, SLCO1B1 and SLCO2B1 polymorphisms influences chloroquine and primaquine treatment in Plasmodium vivax malaria.
    Pharmacogenomics, 2017, Volume: 18, Issue:15

    Topics: Adult; Antimalarials; Brazil; Chloroquine; Drug Therapy, Combination; Female; Genotype; Humans; Live

2017
Large-scale Artemisinin-Piperaquine Mass Drug Administration With or Without Primaquine Dramatically Reduces Malaria in a Highly Endemic Region of Africa.
    Clinical infectious diseases : an official publication of the Infectious Diseases Society of America, 2018, 11-13, Volume: 67, Issue:11

    Topics: Adolescent; Adult; Antimalarials; Artemisinins; Child; Child, Preschool; Comoros; DNA, Protozoan; Dr

2018
Use of poly(amidoamine) drug conjugates for the delivery of antimalarials to Plasmodium.
    Journal of controlled release : official journal of the Controlled Release Society, 2014, Mar-10, Volume: 177

    Topics: Animals; Antimalarials; Chloroquine; Drug Carriers; Erythrocytes; Female; Malaria; Mice; Mice, Inbre

2014
Paucity of Plasmodium vivax mature schizonts in peripheral blood is associated with their increased cytoadhesive potential.
    The Journal of infectious diseases, 2014, May-01, Volume: 209, Issue:9

    Topics: Antimalarials; Cell Adhesion; Chloroquine; Erythrocytes; Humans; Malaria, Vivax; Parasitemia; Plasmo

2014
Transient lesion in the splenium of the corpus callosum in acute uncomplicated falciparum malaria.
    The American journal of tropical medicine and hygiene, 2014, Volume: 90, Issue:6

    Topics: Acute Disease; Adult; Antimalarials; Artemisinins; Chloroquine; Corpus Callosum; Drug Therapy, Combi

2014
A case of quadruple malaria infection imported from Mozambique to Japan.
    The American journal of tropical medicine and hygiene, 2014, Volume: 90, Issue:6

    Topics: Adult; Antimalarials; Artemether, Lumefantrine Drug Combination; Artemisinins; Base Sequence; Coinfe

2014
Causal prophylactic efficacy of primaquine, tafenoquine, and atovaquone-proguanil against Plasmodium cynomolgi in a rhesus monkey model.
    The Journal of parasitology, 2014, Volume: 100, Issue:5

    Topics: Aminoquinolines; Animals; Antimalarials; Atovaquone; Disease Models, Animal; Drug Combinations; Maca

2014
Imported malaria in a non-endemic area: the experience of the university of Campinas hospital in the Brazilian Southeast.
    Malaria journal, 2014, Jul-22, Volume: 13

    Topics: Acquired Immunodeficiency Syndrome; Adolescent; Adult; Anemia; Antimalarials; Artemether; Artemisini

2014
Preparation, characterization, and optimization of primaquine-loaded solid lipid nanoparticles.
    International journal of nanomedicine, 2014, Volume: 9

    Topics: Animals; Antimalarials; Drug Carriers; Emulsions; Lipids; Malaria; Mice; Nanoparticles; Parasitemia;

2014
[Epidemiological characteristics of malaria in the village of Corail, Grand'Anse, Haiti].
    Bulletin de la Societe de pathologie exotique (1990), 2014, Volume: 107, Issue:5

    Topics: Adolescent; Adult; Aged; Antimalarials; Asymptomatic Diseases; Child; Child, Preschool; Chloroquine;

2014
Optimally timing primaquine treatment to reduce Plasmodium falciparum transmission in low endemicity Thai-Myanmar border populations.
    Malaria journal, 2009, Jul-15, Volume: 8

    Topics: Animals; Antimalarials; Asian People; Endemic Diseases; Humans; Malaria, Falciparum; Models, Biologi

2009
Clinical and laboratory features of human Plasmodium knowlesi infection.
    Clinical infectious diseases : an official publication of the Infectious Diseases Society of America, 2009, Sep-15, Volume: 49, Issue:6

    Topics: Adolescent; Adult; Aged; Animals; Antimalarials; Blood Chemical Analysis; Chloroquine; Female; Hemog

2009
Recurrent parasitemias and population dynamics of Plasmodium vivax polymorphisms in rural Amazonia.
    The American journal of tropical medicine and hygiene, 2009, Volume: 81, Issue:6

    Topics: Animals; Antimalarials; Brazil; Chloroquine; Drug Resistance; Haplotypes; Humans; Malaria, Vivax; Mi

2009
Flow cytometry for the evaluation of anti-plasmodial activity of drugs on Plasmodium falciparum gametocytes.
    Malaria journal, 2010, Feb-11, Volume: 9

    Topics: Anti-Infective Agents; Antimalarials; Artemisinins; Chloroquine; Drug Evaluation, Preclinical; Flow

2010
Rapid and effective malaria control in Cambodia through mass administration of artemisinin-piperaquine.
    Malaria journal, 2010, Feb-23, Volume: 9

    Topics: Administration, Oral; Adolescent; Adult; Anti-Infective Agents; Antimalarials; Artemisinins; Cambodi

2010
Revisiting the circulation time of Plasmodium falciparum gametocytes: molecular detection methods to estimate the duration of gametocyte carriage and the effect of gametocytocidal drugs.
    Malaria journal, 2010, May-24, Volume: 9

    Topics: Adolescent; Amodiaquine; Antimalarials; Artemether, Lumefantrine Drug Combination; Artemisinins; Art

2010
Dynamics of Plasmodium falciparum parasitemia regarding combined treatment regimens for acute uncomplicated malaria, Antioquia, Colombia.
    The American journal of tropical medicine and hygiene, 2010, Volume: 83, Issue:1

    Topics: Administration, Oral; Animals; Antimalarials; Artemisinins; Artesunate; Clinical Protocols; Colombia

2010
Design and evaluation of primaquine-artemisinin hybrids as a multistage antimalarial strategy.
    Antimicrobial agents and chemotherapy, 2011, Volume: 55, Issue:10

    Topics: Animals; Antimalarials; Artemisinins; Cell Line; Humans; Malaria; Mice; Parasitemia; Plasmodium berg

2011
In vivo sensitivity monitoring of chloroquine for the treatment of uncomplicated vivax malaria in four bordered provinces of Thailand during 2009-2010.
    Journal of vector borne diseases, 2011, Volume: 48, Issue:4

    Topics: Adolescent; Adult; Aged; Aged, 80 and over; Antimalarials; Child; Child, Preschool; Chloroquine; Dru

2011
Use of a rhesus Plasmodium cynomolgi model to screen for anti-hypnozoite activity of pharmaceutical substances.
    The American journal of tropical medicine and hygiene, 2012, Volume: 86, Issue:6

    Topics: Animals; Antimalarials; Chloroquine; Disease Models, Animal; Drug Evaluation, Preclinical; Macaca mu

2012
Blood schizontocidal activity of WR 238605 (Tafenoquine) against Plasmodium cynomolgi and Plasmodium fragile infections in rhesus monkeys.
    Acta tropica, 2003, Volume: 86, Issue:1

    Topics: Aminoquinolines; Animals; Antimalarials; Female; Macaca mulatta; Malaria; Male; Monkey Diseases; Par

2003
Correlation between Plasmodium vivax variants in Belém, Pará State, Brazil and symptoms and clearance of parasitaemia.
    The Brazilian journal of infectious diseases : an official publication of the Brazilian Society of Infectious Diseases, 2003, Volume: 7, Issue:3

    Topics: Animals; Antimalarials; Brazil; Chloroquine; Genetic Variation; Genotype; Humans; Malaria, Vivax; Pa

2003
Assessment of therapeutic efficacy of chloroquine for vivax malaria in Thailand.
    The Southeast Asian journal of tropical medicine and public health, 2004, Volume: 35, Issue:3

    Topics: Adolescent; Adult; Aged; Aged, 80 and over; Animals; Antimalarials; Child; Chloroquine; Drug Resista

2004
Diagnostic and therapeutic pitfalls associated with primaquine-tolerant Plasmodium vivax.
    Journal of clinical microbiology, 2005, Volume: 43, Issue:2

    Topics: Adult; Animals; Antimalarials; Chemoprevention; Drug Resistance; Humans; Malaria, Vivax; Male; Milit

2005
Cytoplasmic remodeling of erythrocyte raft lipids during infection by the human malaria parasite Plasmodium falciparum.
    Blood, 2007, Sep-15, Volume: 110, Issue:6

    Topics: Animals; Annexin A5; Blotting, Western; Cell Membrane; Cytoplasm; Endocytosis; Erythrocyte Membrane;

2007
Formulation, antimalarial activity and biodistribution of oral lipid nanoemulsion of primaquine.
    International journal of pharmaceutics, 2008, Jan-22, Volume: 347, Issue:1-2

    Topics: Administration, Oral; Animals; Antimalarials; Disease Models, Animal; Drug Stability; Emulsions; Lip

2008
Subclinical avian malaria infections in African black-footed penguins (Spheniscus demersus) and induction of parasite recrudescence.
    Journal of wildlife diseases, 1994, Volume: 30, Issue:3

    Topics: Animals; Animals, Zoo; Baltimore; Birds; Chloroquine; Dexamethasone; Ducks; Immunosuppression Therap

1994
Preliminary evaluation of primaquine activity on rodent malaria model after transdermal administration.
    Parasite (Paris, France), 1997, Volume: 4, Issue:1

    Topics: Administration, Cutaneous; Animals; Antimalarials; Disease Models, Animal; Drug Evaluation; Malaria;

1997
Studies on a primaquine-tolerant strain of Plasmodium vivax from Brazil in Aotus and Saimiri monkeys.
    The Journal of parasitology, 1997, Volume: 83, Issue:4

    Topics: Animals; Anopheles; Antimalarials; Aotidae; Brazil; Chloroquine; Disease Models, Animal; Drug Resist

1997
Primaquine-tolerant vivax malaria in Thailand.
    Annals of tropical medicine and parasitology, 1997, Volume: 91, Issue:8

    Topics: Adult; Antimalarials; Chloroquine; Drug Resistance; Drug Therapy, Combination; Female; Follow-Up Stu

1997
Rodent malaria prophylaxis by transdermal delivery of primaquine.
    International journal for parasitology, 1998, Volume: 28, Issue:8

    Topics: Administration, Cutaneous; Animals; Antimalarials; Drug Evaluation, Preclinical; Malaria; Mice; Para

1998
[Effect of primaquine on the elimination of sexual forms of Plasmodium falciparum in vivo].
    Revista cubana de medicina tropical, 1994, Volume: 46, Issue:3

    Topics: Animals; Antimalarials; Drug Administration Schedule; Humans; Malaria, Falciparum; Parasitemia; Plas

1994
Azithromycin: antimalarial profile against blood- and sporozoite-induced infections in mice and monkeys.
    Experimental parasitology, 2000, Volume: 94, Issue:1

    Topics: Animals; Anti-Bacterial Agents; Antimalarials; Azithromycin; Chloroquine; Doxycycline; Erythromycin;

2000
Screening of five drugs for efficacy against Babesia felis in experimentally infected cats.
    Journal of the South African Veterinary Association, 2000, Volume: 71, Issue:1

    Topics: Animals; Anti-Infective Agents; Antiprotozoal Agents; Babesiosis; Cat Diseases; Cats; Drug Combinati

2000
Are avian blood parasites pathogenic in the wild? A medication experiment in blue tits (Parus caeruleus).
    Proceedings. Biological sciences, 2000, Dec-22, Volume: 267, Issue:1461

    Topics: Animals; Animals, Wild; Bird Diseases; Birds; Eukaryota; Parasitemia; Primaquine; Protozoan Infectio

2000
Asexual erythrocytic forms of Plasmodium falciparum in asymptomatic American and Korean soldiers serving in Vietnam.
    Military medicine, 1967, Volume: 132, Issue:2

    Topics: Animals; Antimalarials; Australia; Chloroquine; Erythrocytes; Humans; Korea; Malaria, Falciparum; Mi

1967