benserazide and Parkinson Disease studies

Benserazide: An inhibitor of DOPA DECARBOXYLASE that does not enter the central nervous system. It is often given with LEVODOPA in the treatment of parkinsonism to prevent the conversion of levodopa to dopamine in the periphery, thereby increasing the amount that reaches the central nervous system and reducing the required dose. It has no antiparkinson actions when given alone.
benserazide : A carbohydrazide that results from the formal condensation of the carboxy group of DL-serine with the primary amino group of 4-(hydrazinylmethyl)benzene-1,2,3-triol. An aromatic-L-amino-acid decarboxylase inhibitor (DOPA decarboxylase inhibitor) that does not enter the central nervous system, it is used as its hydrochloride salt as an adjunct to levodopa in the treatment of parkinsonism. By preventing the conversion of levodopa to dopamine in the periphery, it causes an increase in the amount of levodopa reaching the central nervous system and so reduces the required dose. Benserazide has no antiparkinson actions when given alone.

Parkinson Disease: A progressive, degenerative neurologic disease characterized by a TREMOR that is maximal at rest, retropulsion (i.e. a tendency to fall backwards), rigidity, stooped posture, slowness of voluntary movements, and a masklike facial expression. Pathologic features include loss of melanin containing neurons in the substantia nigra and other pigmented nuclei of the brainstem. LEWY BODIES are present in the substantia nigra and locus coeruleus but may also be found in a related condition (LEWY BODY DISEASE, DIFFUSE) characterized by dementia in combination with varying degrees of parkinsonism. (Adams et al., Principles of Neurology, 6th ed, p1059, pp1067-75)

Research Excerpts

Excerpt	Relevance	Reference
"This study determined the effects of single doses of opicapone (OPC), a novel third-generation catechol-O-methyltransferase (COMT) inhibitor, on levodopa and 3-O-methyl-levodopa (3-OMD) pharmacokinetics (PK), COMT activity and motor fluctuations in patients with Parkinson disease (PD)."	9.22	Effect of 3 Single-Dose Regimens of Opicapone on Levodopa Pharmacokinetics, Catechol-O-Methyltransferase Activity and Motor Response in Patients With Parkinson Disease. ( Almeida, L; Falcão, A; Ferreira, JJ; Nunes, T; Pinto, R; Rocha, JF; Santos, A; Soares-da-Silva, P, 2016)
"The aims of the present study were to investigate the pharmacokinetic and pharmacodynamic (pk/pd) relationship of levodopa (l-dopa) in patients with advanced Parkinson disease (PD) and also to evaluate the effect of tolcapone on the pk/pd analysis of l-dopa in 1 patient with severe dyskinesias and fluctuations."	9.14	Pharmacokinetic-pharmacodynamic modeling of levodopa in patients with advanced Parkinson disease. ( Adamiak, U; Bialecka, M; Gawronska-Szklarz, B; Kaldonska, M; Klodowska-Duda, G; Safranow, K; Wyska, E, 2010)
"A sixteen-week study examined the effect of Madopa and Sinemet on patients with Parkinson disease disease suffering nausea or vomiting as side-effects of levodopa therapy and compared the efficacy of the three preparations in controlling the symptoms of Parkinson disease."	9.04	A double-blind comparison of levodopa, Madopa, and Sinemet in Parkinson disease. ( Diamond, SG; Markham, CH; Treciokas, LJ, 1978)
"Plasma levodopa and therapeutic responses to treatment with levodopa in combination with benserazide or carbidopa were studied in 49 patients with Parkinson disease not previously treated with levodopa in a blind randomized crossover trial."	9.04	Levodopa with benserazide or carbidopa in Parkinson disease. ( Mölsä, P; Rinne, UK, 1979)
"A retrospective cohort study of 21 patients on levodopa/benserazide and one patient on levodopa-carbidopa intestinal gel with clinically suspected or biopsy proven microscopic colitis."	8.02	Levodopa/dopa decarboxylase inhibitor associated microscopic colitis: An under-recognized drug reaction. ( Babu, S; Chang, FC; Dal, S; Fletcher, N; Fung, VSC; Mahant, N; Martin, AJ; Morales-Briceno, H; Nankervis, J; Ong, TL; Robbie, M; Williams, LJ, 2021)
"This study aims to investigate hyperhomocysteinemia (HHcy) resulted from treatment in patients with Parkinson's disease (PD) and to evaluate the therapeutic outcome of HHcy."	7.83	The effect of levodopa benserazide hydrochloride on homocysteinemia levels in patients with Parkinson's disease and treatment of hyperhomocysteinemia. ( Cao, LD; Guo, G; Wu, QY; Xu, S, 2016)
"For many patients with Parkinson disease and levodopa-related motor fluctuations, the latency to onset of action of a single dose of a levodopa preparation may be both long and variable."	7.68	The clinical efficacy of single morning doses of levodopa methyl ester: dispersible Madopar and Sinemet plus in Parkinson disease. ( Bramante, L; Quinn, NP; Ruggieri, S; Steiger, MJ; Stocchi, F, 1992)
" The main levodopa pharmacodynamic variables were the maximum percentage increase in tapping frequency over baseline values (ΔTapmax %) and the area under the tapping effect-time curve (AUCTap)."	5.43	Pharmacodynamics of a low subacute levodopa dose helps distinguish between multiple system atrophy with predominant Parkinsonism and Parkinson's disease. ( Calandra-Buonaura, G; Capellari, S; Contin, M; Cortelli, P; Doria, A; Guaraldi, P; Lopane, G; Martinelli, P, 2016)
"Pramipexole is a non-ergot dopamine agonist that is used frequently as a single therapy or in combination for the management of Parkinson's disease."	5.38	Pramipexole-related chronic lower limb oedema in a patient with Parkinson's disease. ( Munhoz, RP; Teive, HA; Zavala, JA, 2012)
" Two dosage strengths are available: 100 mg levodopa plus 25 mg benserazide and 50 mg levodopa plus 12."	5.29	[Benefits of a new galenic form of levodopa and benserazide in the treatment of patients with Parkinson disease]. ( Dessibourg, CA; Gachoud, JP, 1995)
" Due to a lower bioavailability of the slow release formulation--the latter is based on the "hydrodynamically balanced system" (HBS)--, the patients remained initially on their time schedule of drug intake but received a higher dose of L-DOPA slow release compared to the preceding L-DOPA standard therapy."	5.29	[Effectiveness of slow release L-DOPA/benserazide in treatment of end-of-dose akinesia in Parkinson disease]. ( Eichhorn, TE; Kohnen, R; Oertel, WH; Poewe, W; Schrag, A; Selzer, R; Trenkwalder, C, 1995)
"This study determined the effects of single doses of opicapone (OPC), a novel third-generation catechol-O-methyltransferase (COMT) inhibitor, on levodopa and 3-O-methyl-levodopa (3-OMD) pharmacokinetics (PK), COMT activity and motor fluctuations in patients with Parkinson disease (PD)."	5.22	Effect of 3 Single-Dose Regimens of Opicapone on Levodopa Pharmacokinetics, Catechol-O-Methyltransferase Activity and Motor Response in Patients With Parkinson Disease. ( Almeida, L; Falcão, A; Ferreira, JJ; Nunes, T; Pinto, R; Rocha, JF; Santos, A; Soares-da-Silva, P, 2016)
"The aims of the present study were to investigate the pharmacokinetic and pharmacodynamic (pk/pd) relationship of levodopa (l-dopa) in patients with advanced Parkinson disease (PD) and also to evaluate the effect of tolcapone on the pk/pd analysis of l-dopa in 1 patient with severe dyskinesias and fluctuations."	5.14	Pharmacokinetic-pharmacodynamic modeling of levodopa in patients with advanced Parkinson disease. ( Adamiak, U; Bialecka, M; Gawronska-Szklarz, B; Kaldonska, M; Klodowska-Duda, G; Safranow, K; Wyska, E, 2010)
"A sixteen-week study examined the effect of Madopa and Sinemet on patients with Parkinson disease disease suffering nausea or vomiting as side-effects of levodopa therapy and compared the efficacy of the three preparations in controlling the symptoms of Parkinson disease."	5.04	A double-blind comparison of levodopa, Madopa, and Sinemet in Parkinson disease. ( Diamond, SG; Markham, CH; Treciokas, LJ, 1978)
"Plasma levodopa and therapeutic responses to treatment with levodopa in combination with benserazide or carbidopa were studied in 49 patients with Parkinson disease not previously treated with levodopa in a blind randomized crossover trial."	5.04	Levodopa with benserazide or carbidopa in Parkinson disease. ( Mölsä, P; Rinne, UK, 1979)
"A retrospective cohort study of 21 patients on levodopa/benserazide and one patient on levodopa-carbidopa intestinal gel with clinically suspected or biopsy proven microscopic colitis."	4.02	Levodopa/dopa decarboxylase inhibitor associated microscopic colitis: An under-recognized drug reaction. ( Babu, S; Chang, FC; Dal, S; Fletcher, N; Fung, VSC; Mahant, N; Martin, AJ; Morales-Briceno, H; Nankervis, J; Ong, TL; Robbie, M; Williams, LJ, 2021)
"This study aims to investigate hyperhomocysteinemia (HHcy) resulted from treatment in patients with Parkinson's disease (PD) and to evaluate the therapeutic outcome of HHcy."	3.83	The effect of levodopa benserazide hydrochloride on homocysteinemia levels in patients with Parkinson's disease and treatment of hyperhomocysteinemia. ( Cao, LD; Guo, G; Wu, QY; Xu, S, 2016)
" The present results show beneficial antioxidant and methyl donor properties of betaine versus oxidative stress and hyperhomocysteinemia induced by levodopa and benserazide in an animal model."	3.81	Beneficial antioxidant properties of betaine against oxidative stress mediated by levodopa/benserazide in the brain of rats. ( Alirezaei, M; Dezfoulian, O; Khoshdel, Z; Rashidipour, M; Taghadosi, V, 2015)
" The aims of this study were therefore (1) to investigate the anti-dyskinetic effects of piribedil on L-DOPA-induced contralateral turning behaviour, locomotive dyskinesias (LD), axial dystonia (AD), orolingual dyskinesia (OD) and forelimb dyskinesia (FD) and (2) to compare these effects to the α(2) adrenoceptor antagonist, idazoxan, or the α(2) adrenoceptor agonist, clonidine."	3.79	The effect of piribedil on L-DOPA-induced dyskinesias in a rat model of Parkinson's disease: differential role of α(2) adrenergic mechanisms. ( Gerlach, M; Halley, P; Riederer, P; van den Buuse, M, 2013)
"For many patients with Parkinson disease and levodopa-related motor fluctuations, the latency to onset of action of a single dose of a levodopa preparation may be both long and variable."	3.68	The clinical efficacy of single morning doses of levodopa methyl ester: dispersible Madopar and Sinemet plus in Parkinson disease. ( Bramante, L; Quinn, NP; Ruggieri, S; Steiger, MJ; Stocchi, F, 1992)
"Parkinsonian patients with orthostatic hypotension and dizziness due to usual antiparkinson therapy have been treated with the precursor amino-acid of noradrenaline, DL-3,4-threo-dihydroxyphenylserine (DL-3,4-threo-DOPS)."	3.66	DL-3,4-threo-DOPS in Parkinson's disease: effects on orthostatic hypotension and dizziness. ( Birkmayer, G; Birkmayer, W; Lechner, H; Riederer, P, 1983)
"The changes in prolactin release induced by acute doses of L-Dopa + benserazide (250 mg) were analysed in Parkinson disease patients undergoing various drug treatments."	3.66	[Exploration of the tubero-hypophyseal dopaminergic system in patients with chronic parkinsonism during chronic treatment with L-DOPA]. ( Baldassarre, G; Fazio, B, 1983)
"In four patients with Parkinson disease, we compared carbidopa combined with levodopa (Sinemet) and benserazide combined with levodopa (Madopar)."	3.66	Comparative effectiveness of two extracerebral DOPA decarboxylase inhibitors in Parkinson disease. ( Estey, E; Goldstein, M; Gopinathan, G; Lieberman, A; Ohashi, T; Sauter, A, 1978)
"The relationship between dopamine receptor stimulation by bromocriptine or levodopa and the relief of parkinsonism was studied in 24 patients with Parkinson disease."	3.66	Brain dopamine receptor stimulation and the relief of Parkinsonism: relationship between bromocriptine and levodopa. ( Marttila, R; Rinne, UK, 1978)
"While several generic preparations of levodopa/carbidopa and levodopa/benserazide (LBD) are currently available, pharmacokinetic (PK) equivalence and therapeutic equivalence studies with levodopa generics are not available in Italy."	2.90	Clinical and pharmacokinetics equivalence of multiple doses of levodopa benserazide generic formulation vs the originator (Madopar). ( Alessandroni, J; Bonassi, S; Bravi, D; Casali, M; Fossati, C; Grassini, P; Ialongo, C; Onofrj, M; Radicati, FG; Stocchi, F; Torti, M; Vacca, L, 2019)
"Micrographia is a common symptom in Parkinson's disease, which manifests as either a consistent or progressive reduction in the size of handwriting or both."	2.82	Neural correlates underlying micrographia in Parkinson's disease. ( Chan, P; Feng, T; Hallett, M; Hou, Y; Wu, T; Zhang, J, 2016)
"Two levodopa tests were performed, one at baseline and another following the maintenance phase."	2.80	Effect of opicapone on levodopa pharmacokinetics, catechol-O-methyltransferase activity and motor fluctuations in patients with Parkinson's disease. ( Falcão, A; Ferreira, JJ; Nunes, T; Pinto, R; Rocha, JF; Santos, A; Soares-da-Silva, P, 2015)
" Reported adverse events were comparable between LB and LC users."	2.80	Efficacy and safety of entacapone in levodopa/carbidopa versus levodopa/benserazide treated Parkinson's disease patients with wearing-off. ( Kuoppamäki, M; Leinonen, M; Poewe, W, 2015)
" Adverse effects from Western drug-based medical intervention prevent long-term adherence to these therapies in many patients."	2.78	Evaluation on the efficacy and safety of Chinese herbal medication Xifeng Dingchan Pill in treating Parkinson's disease: study protocol of a multicenter, open-label, randomized active-controlled trial. ( Ma, YZ; Shen, XM; Zhang, J, 2013)
"Oral levodopa dosing was increased in 28% of patients; the primary outcome remained significant when these patients were excluded."	2.75	Direct switch from levodopa/benserazide or levodopa/carbidopa to levodopa/carbidopa/entacapone in Parkinson's disease patients with wearing-off: efficacy, safety and feasibility--an open-label, 6-week study. ( Amar, K; Eggert, K; Kuoppamäki, M; Leinonen, M; Luotonen, L; Nissinen, H; Oertel, W; Skogar, O, 2010)
"Other efficacy variables (Unified Parkinson's Disease Rating Scale II, III, and IVb and Investigator's Global Assessment scores) improved significantly after switching to tolcapone."	2.75	Replacing a dopamine agonist by the COMT-inhibitor tolcapone as an adjunct to L-dopa in the treatment of Parkinson's disease: a randomized, multicenter, open-label, parallel-group study. ( Eggert, K; Eichhorn, T; Oertel, WH; Ries, V; Selzer, R, 2010)
"Treatment with levodopa/carbidopa/entacapone resulted in significantly greater improvements in PDQ-8 scores compared to treatment with levodopa/carbidopa (mean difference 1."	2.74	Quality of life in early Parkinson's disease treated with levodopa/carbidopa/entacapone. ( Fung, VS; Herawati, L; Wan, Y, 2009)
"Fifty cases in a treatment group were treated by acupuncture combined with madopar, and 30 cases in a control group treated by madopar only."	2.73	Fifty cases of Parkinson's disease treated by acupuncture combined with madopar. ( Ren, XM, 2008)
" Long-term levodopa administration results in an increased levodopa plasma bioavailability in PD patients."	2.71	Chronic levodopa intake increases levodopa plasma bioavailability in patients with Parkinson's disease. ( Muhlack, S; Müller, T; Przuntek, H; Twiehaus, S; Welnic, J; Woitalla, D, 2004)
" The main levodopa pharmacokinetic outcome variables were time to peak and peak plasma concentration, plasma elimination half-life, and the area under the plasma concentration-time curve."	2.71	Genetic polymorphism of catechol-O-methyltransferase and levodopa pharmacokinetic-pharmacodynamic pattern in patients with Parkinson's disease. ( Albani, F; Baruzzi, A; Contin, M; Martinelli, P; Mochi, M; Riva, R, 2005)
" Inhibition of catechol-O-methyltransferase by tolcapone has been shown to increase levodopa bioavailability and plasma elimination half life, thereby prolonging the efficacy of levodopa."	2.69	Catechol-O-methyltransferase inhibition with tolcapone reduces the "wearing off" phenomenon and levodopa requirements in fluctuating parkinsonian patients. ( Baas, H; Beiske, AG; Ghika, J; Jackson, M; Oertel, WH; Poewe, W; Ransmayr, G, 1998)
"When tolcapone was combined with 25 mg benserazide the elevation was small."	2.69	The effect of tolcapone on the pharmacokinetics of benserazide. ( Beiske, A; Fotteler, B; Jorga, KM; Larsen, JP; Moe, B; Schleimer, M; Schmitt, M, 1999)
" Tolcapone increased the bioavailability (AUC 0-infinity) and apparent elimination half-life (t(1/2)) of levodopa by 80 and 40%, respectively, compared to placebo."	2.69	COMT inhibition by tolcapone further improves levodopa pharmacokinetics when combined with a dual-release formulation of levodopa/benserazide. A novel principle in the treatment of Parkinson's disease. ( Crevoisier, C; Gasser, UE; Hovens, SE; Jorga, K; van Giersbergen, PL, 1999)
"The pharmacokinetic model which best described the data was a two-compartment open model with first-order absorption and possibly a lag-time."	2.69	Population pharmacokinetics of tolcapone in parkinsonian patients in dose finding studies. ( Banken, L; Fotteler, B; Jorga, K; Snell, P; Steimer, JL, 2000)
"Treatment with levodopa and dopa decarboxylase inhibitor (arm 1) or levodopa and decarboxylase inhibitor in combination with selegiline (arm 2)."	2.68	Comparison of therapeutic effects and mortality data of levodopa and levodopa combined with selegiline in patients with early, mild Parkinson's disease. Parkinson's Disease Research Group of the United Kingdom. ( Lees, AJ, 1995)
"Tremor was assessed via accelerometry and surface EMG."	2.68	'Atypical' tremor. ( Byth, K; Einstein, R; Henderson, JM; Jackson, DM; Morris, JG, 1995)
" The drugs were dosed according to the individual need of the patients."	2.68	Sustained-release Madopar HBS compared with standard Madopar in the long-term treatment of de novo parkinsonian patients. ( Andersen, A; Boas, J; Boisen, E; Borgmann, R; Buch, D; Dupont, E; Helgetveit, AC; Kjaer, MO; Kristensen, TN; Mikkelsen, B; Pakkenberg, H; Presthus, J; Stien, R; Worm-Petersen, J, 1996)
"5%, probably reflecting some differences in the bioavailability of the various galenical formulations, and the mean daily drug intakes were reduced from 5."	2.68	Clinical efficacy and tolerability of a new levodopa/benserazide dual-release formulation in parkinsonian patients. L-Dopa Dual-Release Study Group. ( Gachoud, JP; Gasser, U; Ghika, J, 1997)
"Ten patients with a diagnosis of idiopathic Parkinson's disease and motor fluctuations otherwise unresponsive to conventional therapy were selected."	2.67	[A new levodopa benserazide preparation for Parkinson's disease with motor fluctuations refractory to standard L-dopa]. ( Casas Parera, I; Diaz, S; Fernández Pardal, MM; Gatto, E; Micheli, F, 1991)
" The present study, therefore, compared single dose kinetics and pharmacodynamic effects of three dosages of L-dopa/bensearazid-s."	2.67	[Slow-release L-dopa vs. standard L-dopa in Parkinson patients in various stages of the disease. Studies of pharmacokinetics and motor effectiveness]. ( Baas, H; Bergemann, N; Fischer, PA, 1994)
"Patients with Parkinson's disease (PD) are more dependent on visual information during movements than normals."	2.67	Visual control of arm movement in Parkinson's disease. ( Dichgans, J; Klockgether, T, 1994)
"In the Parkinson's disease group studied, the frequency, EMG pattern of bursts, and response to L-Dopa were similar for the two tremors (median improvement of RT by 70% and PT by 61%)."	2.67	Postural tremor of Parkinson's disease. ( Byth, K; Einstein, R; Henderson, JM; Jackson, D; Morris, JG; Yiannikas, C, 1994)
" The results of the substitution phase show that combined treatment permitted a mean reduction of the levodopa dosage by 40%, without deterioration of therapeutic response."	2.67	Primary combination therapy of early Parkinson's disease. A long-term comparison between the combined regimen bromocriptine/levodopa and levodopa monotherapy--first interim report. ( Kraus, PH; Letzel, H; Przuntek, H; Schwarzmann, D; Welzel, D, 1992)
"20 patients with Parkinson's disease and a fluctuating response to chronic treatment with conventional L-dopa preparations participated in an open randomized trial comparing two sustained-release L-dopa preparations (Madopar HBS, Sinemet CR4)."	2.67	Comparative efficacy of two oral sustained-release preparations of L-dopa in fluctuating Parkinson's disease. Preliminary findings in 20 patients. ( Kleedorfer, B; Poewe, W, 1992)
"Temazepam was consistently less potent than chlormethiazole on tests of drowsiness and psychomotor performance."	2.67	A single-dose study of the pharmacodynamic effects of chlormethiazole, temazepam and placebo in elderly parkinsonian patients. ( Ashwood, TJ; Bateman, DN; Tulloch, JA; Woodhouse, KW, 1991)
" The equivalent L-dopa dosage had to be increased by 56% (29-100%) with Madopar HBS while mean dopamine levels increased in four patients (by 47-257%) without the occurrence of peripheral side-effects."	2.67	Controlled-release levodopa/benserazide (Madopar HBS): clinical observations and levodopa and dopamine plasma concentrations in fluctuating parkinsonian patients. ( Ceballos-Baumann, AO; Eckert, W; von Kummer, R; Weicker, H, 1990)
" The mean optimum total daily dosage of conventional Madopar was 820 mg taken in a mean of 6."	2.67	A comparison of the effects of controlled-release levodopa (Madopar CR) with conventional levodopa in late Parkinson's disease. ( Blackburn, NA; Boddie, HG; Ellis, CJ; Kendal, BR; MacMahon, DG; Sachdev, D, 1990)
" In 13 patients a considerable diminution in nocturnal akinesia and in the frequency of waking up was reached with a mean dosage of 308 mg of Madopar HBS."	2.67	Madopar HBS in nocturnal symptoms of Parkinson's disease. ( Jansen, EN; Meerwaldtt, JD, 1990)
" The results suggest, the BH4 in the dosage used, is not effective in the treatment of Parkinson's disease."	2.66	Tetrahydrobiopterin and Parkinson's disease. ( Dissing, IC; Gerdes, AM; Güttler, F; Lou, H; Lykkelund, C; Pakkenberg, H; Rasmussen, V, 1989)
" Even better results could be accomplished in an extended trial attempting to establish the best dosage ratio of the combination, possibly admitting increased dosage."	2.66	A combined regimen of subcutaneous lisuride and oral Madopar HBS in Parkinson's disease. ( Aljanati, R; Caamaño, JL; Chouza, C; de Medina, O; Romero, S; Scaramelli, A, 1988)
"Of the three main symptoms of Parkinson's disease, the best effect was seen on tremor, and less pronounced effects on bradykinesia and rigidity."	2.66	Adjuvant treatment of Parksinson's disease with budipine: a double-blind trial versus placebo. ( Bliesath, H; Jellinger, K, 1987)
" During the first month the dosage titration was aimed at finding the optimal therapeutic effect."	2.66	Clinical trial of Madopar HBS in parkinsonian patients with fluctuating drug response after long-term levodopa therapy. ( Aymard, N; Holzer, J; Rondot, P; Ziegler, M, 1987)
"In a open study in 13 patients with Parkinson's disease with 'on-off' fluctuations, all (n = 3) or part (n = 10) of the usual intake of levodopa (with peripheral decarboxylase inhibitor) was replaced by Madopar HBS for 5-122 days (median 35)."	2.66	Open study of Madopar HBS, a new formulation of levodopa with benserazide, in 13 patients with Parkinson's disease and 'on-off' fluctuations. ( Marion, MH; Marsden, CD; Quinn, NP, 1987)
" The clinical response to Madopar HBS was delayed and brief; the relative bioavailability was only 50%."	2.66	Single-dose studies of a slow-release preparation of levodopa and benserazide (Madopar HBS) in Parkinson's disease. ( Jenner, P; Malcolm, SL; Marion, MH; Marsden, CD; Quinn, NP; Stocchi, F, 1987)
" At the beginning the patients were switched from standard Madopar to Madopar HBS, initially keeping constant L-dopa dosage and the number of daily doses."	2.66	Open clinical study of Madopar HBS. ( Ludin, HP, 1987)
" However, with the new formulation the dosage had to be increased by 86% on average as compared with standard Madopar."	2.66	Treatment of parkinsonian conditions with a controlled-release form of levodopa--preliminary study. ( D'Andrea, G; Durisotti, C; Ferro-Milone, F; Lion, P; Lorizio, A; Nordera, GP, 1987)
" For the first few days (up to 1 week) dosage and number of daily intakes of HBS were the same as those of the standard formulation."	2.66	Preliminary experience with Madopar HBS: clinical observations and plasma levodopa concentrations. ( Baas, H; Fischer, PA, 1987)
" The overall increase in dosage of levodopa with Madopar HBS was 54% in comparison with the initial standard Madopar dosage."	2.66	Open multicenter trial with Madopar HBS in parkinsonian patients. Preliminary assessment after short-term treatment. ( Heersema, T; Jansen, EN; Meerwaldt, JD; Speelman, JD; van Manen, J, 1987)
"In 3 patients with longstanding Parkinson's disease treated with Madopar or Nacom, who were not included in the study, the doses of the above drugs could be maintained or reduced by addition of deprenyl."	2.66	Levodopa and monoamine oxidase inhibitor combination therapy. A controlled clinical trial. ( Grundmann, M; Schimrigk, K, 1987)
" The frequency of drug intake was unaltered but daily dosage could be increased by 30% without increasing severity of abnormal movements to a similar degree."	2.66	[Controlled release levodopa-benserazide and changes in efficacy during treatment of Parkinson's disease]. ( Aymard, N; Holzer, J; Rondot, P; Ziegler, M, 1987)
" The dosage of drug was titrated at each visit to give minimum risk with acceptable benefit."	2.66	Patient benefits of l-dopa and a decarboxylase inhibitor in the treatment of Parkinson's disease in elderly patients. ( Admani, AK; Cordingley, GJ; Harris, RI; Verma, S, 1985)
" Subsequently they were treated with either a mean dosage of 444 mg levodopa and benserazide (47 patients) or a combination of a mean of 298 mg levodopa and benserazide plus 17 mg bromocriptine (32 patients)."	2.65	[Combined treatment of the early stages of Parkinson's syndrome with bromocriptine and levodopa. The results of a multicenter study]. ( Fischer, PA; Majer, M; Przuntek, H; Welzel, D, 1984)
" Mean daily maintenance dosage was 612."	2.65	Levodopa/benserazide ('Madopar') combination therapy in elderly patients with parkinsonism. ( Carlyle, D; Williams, BO, 1979)
" With both drugs, Madopar or Sinemet, an optimum therapeutic result was obtained with relatively small doses of L-dopa (the reduction in L-dopa dosage amounting to about 80%)."	2.65	[The combined treatment of Parkinson's disease with L-dopa plus decarboxylase inhibitors (carbidopa, benserazide) (author's transl)]. ( Birkmayer, W; Mentasti, M; Podiwinsky, F; Riederer, P, 1979)
" Patients were allocated at random to treatment with either levodopa + benserazide ratio 4:1 (Madopar) or levodopa + carbidopa ratio 10:1 (Sinemet) using dosage schedules recommended by the manufacturers which they had to adhere to for 6 months."	2.64	Parkinson's disease treated with Sinemet or Madopar. A controlled multicenter trial. ( Birket-Smith, E; Dupont, E; Hansen, E; Mikkelsen, B; Pakkenberg, H; Presthus, J; Rautakorpi, I; Riman, E; Rinne, UK, 1976)
"The treatment of patients suffering from idiopathic Parkinson's disease has become more and more complex."	2.43	[Idiopathic Parkinson's disease: practical hints for the treatment]. ( Ludin, HP, 2005)
"Amantadine has been teratogenic in rats and selegiline has caused neurochemical and behavioral alterations in rats when coadministered with clorgyline."	2.40	Pregnancy in Parkinson's disease: a review of the literature and a case report. ( Hagell, P; Odin, P; Vinge, E, 1998)
" Administration in daily dosage of 10 mgs produces an almost complete inhibition of the enzyme."	2.37	R-(-)-deprenyl and parkinsonism. ( Yahr, MD, 1987)
"Levodopa has been shown to be a safe pharmacologic agent even after long-term usage."	2.35	Levodopa. ( Yahr, MD, 1975)
" The subjects in the control group received only levodopa and benserazide hydrochloride treatment, while the observation group was treated with Resagiline in combination with the clinical control group."	1.91	Effects of rasagiline combined with levodopa and benserazide hydrochloride on motor function and homocysteine and IGF-1 levels in elderly patients with Parkinson's disease. ( Gao, F; Gao, L; Miao, J; Yang, Y, 2023)
" The relationship between the difference in the DCI to levodopa ratio and the development of motor complications in long-term administration of levodopa is unknown."	1.72	The relationship between the distinct ratios of benserazide and carbidopa to levodopa and motor complications in Parkinson's disease: A retrospective cohort study. ( Baba, Y; Futamura, A; Kinno, R; Nabeshima, Y; Nomoto, S; Osakabe, Y; Shoji, D; Takahashi, S; Yasumoto, T, 2022)
"Benserazide is used in the treatment of Parkinson's disease and was noticed to induce gamma globin in preclinical models."	1.62	Benserazide as a potential novel fetal hemoglobin inducer: an observational study in non-carriers of hemoglobin disorders. ( Costa, FF; de Azevedo, PC; Fertrin, KY; Leonardo, DP; Olops, L; Piovesana, LG; Santos, MEHP; Tavares, AHJ; Vendrame, F, 2021)
"Parkinson's disease is clinically defined by bradykinesia, along with rigidity and tremor."	1.56	Effects of dopamine on reinforcement learning in Parkinson's disease depend on motor phenotype. ( Cools, R; den Ouden, HEM; Dirkx, MF; Helmich, RC; Toni, I; van Nuland, AJ; Zach, H, 2020)
"Benserazide is an irreversible inhibitor of peripheral aromatic L-amino acid decarboxylase that prevents the breakdown of levodopa in the bloodstream."	1.48	Nanocarrier for levodopa Parkinson therapeutic drug; comprehensive benserazide analysis. ( Etminan, N; Rahmanifar, E; Yoosefian, M, 2018)
"Re-emergent tremor is a continuation of resting tremor during stable posturing, and it has a dopaminergic basis."	1.48	The nature of postural tremor in Parkinson disease. ( Bloem, BR; Dirkx, MF; Hallett, M; Helmich, RC; Zach, H, 2018)
"The aim of our study was to assess the frailty phenotype prevalence in geriatric inpatients with mild parkinsonian signs (MPS) and to investigate levodopa test in the frail patients with MPS."	1.46	Frailty phenotype and the role of levodopa challenge test in geriatric inpatients with mild parkinsonian signs. ( Bugdol, M; Czernek, M; Derejczyk, J; Kapko, W; Kawa, J; Marcisz, C; Seiffert, P; Stępień-Wyrobiec, O; Szymszal, J; Torbus, A, 2017)
"In this case report, we describe a Parkinson's disease (PD) patient with limb-kinetic apraxia (LKA) in whom degeneration of the corticofugal tract (CFT) from the supplementary motor area (SMA) was observed in diffusion tensor tractography (DTT)."	1.46	Degeneration of the corticofugal tract from the secondary motor area in a Parkinson's disease patient with limb-kinetic apraxia: A case report. ( Chang, MC; Lee, HD, 2017)
" The main levodopa pharmacodynamic variables were the maximum percentage increase in tapping frequency over baseline values (ΔTapmax %) and the area under the tapping effect-time curve (AUCTap)."	1.43	Pharmacodynamics of a low subacute levodopa dose helps distinguish between multiple system atrophy with predominant Parkinsonism and Parkinson's disease. ( Calandra-Buonaura, G; Capellari, S; Contin, M; Cortelli, P; Doria, A; Guaraldi, P; Lopane, G; Martinelli, P, 2016)
"Parkinson's disease is a neurodegenerative disorder characterized by a loss of nigrostriata dopaminergic neurons, which has been thought, at least in part, to result from oxidative stress."	1.43	Neuroprotective effects of stemazole in the MPTP-induced acute model of Parkinson's disease: Involvement of the dopamine system. ( Du, N; Guo, Z; Han, M; Huang, Y; Liu, J; Xu, S, 2016)
"Levodopa (l-DOPA) has been proved to reverse the pathologic neuron activities in many brain regions related to Parkinson's disease (PD)."	1.43	Effect of l-DOPA on local field potential relationship between the pedunculopontine nucleus and primary motor cortex in a rat model of Parkinson's disease. ( Geng, X; Han, H; Hou, Y; Lei, C; Li, M; Wang, M; Wang, X; Xie, J; Yao, X; Zhang, Q; Zhang, X, 2016)
" Rats were dosed orally with Tozadenant, a selective A2A receptor antagonist, and three different doses of Radiprodil, an NR2B-selective NMDA receptor antagonist."	1.42	Behavioural Assessment of the A2a/NR2B Combination in the Unilateral 6-OHDA-Lesioned Rat Model: A New Method to Examine the Therapeutic Potential of Non-Dopaminergic Drugs. ( De Wolf, C; Downey, P; Michel, A; Scheller, D; Schwarting, R; Van Damme, X, 2015)
"Although patients with Parkinson's disease show impairments in cognitive performance even at the early stage of the disease, the synaptic mechanisms underlying cognitive impairment in this pathology are unknown."	1.38	Mechanisms underlying the impairment of hippocampal long-term potentiation and memory in experimental Parkinson's disease. ( Calabresi, P; Costa, C; de Iure, A; Di Filippo, M; Di Luca, M; Gardoni, F; Ghiglieri, V; Latagliata, EC; Marti, M; Morari, M; Pascucci, T; Pendolino, V; Picconi, B; Puglisi-Allegra, S; Sgobio, C; Siliquini, S; Spillantini, MG; Tantucci, M; Tozzi, A, 2012)
"Pramipexole is a non-ergot dopamine agonist that is used frequently as a single therapy or in combination for the management of Parkinson's disease."	1.38	Pramipexole-related chronic lower limb oedema in a patient with Parkinson's disease. ( Munhoz, RP; Teive, HA; Zavala, JA, 2012)
"Psychotic features in patients with Parkinson's Disease usually present as visual hallucinations against a background of cognitive deterioration and dopaminomimetic therapy."	1.36	Isolated delusional syndrome in Parkinson's Disease. ( Bozi, M; Christodoulou, C; Douzenis, A; Gasparinatos, G; Stamboulis, E; Stefanis, C; Stefanis, L; Stefanis, N, 2010)
" Based on the results of rotational behavior and forelimb hyperkinesia in Week 5, the rats were allocated to three treatment groups (saline and two dosing rates of piclozotan set at 0."	1.36	Effects of piclozotan (SUN N4057), a partial serotonin 1A receptor agonist, on motor complications induced by repeated administration of levodopa in parkinsonian rats. ( Inoue, T; Koyama, M; Ogata, A; Tani, Y, 2010)
"We studied 10 Parkinson's disease patients and examined adipose tissue and skeletal muscle metabolism directly with microdialysis."	1.35	Influences of levodopa on adipose tissue and skeletal muscle metabolism in patients with idiopathic Parkinson's disease. ( Adams, F; Boschmann, M; Franke, G; Gottschalk, S; Janke, J; Jordan, J; Kupsch, A; Leisse, MC; Lipp, A; Lobsien, E; Spranger, J, 2008)
"A marked reversal of dystonia was produced in the first seven patients by the withdrawal or dose decrease of dopaminergic PS priming drug, and in the eighth patient an increase of dopaminergic therapy was necessary."	1.35	Reversible Pisa syndrome in patients with Parkinson's disease on dopaminergic therapy. ( Cannas, A; Floris, G; Marrosu, F; Marrosu, MG; Piga, M; Serra, A; Solla, P; Tacconi, P, 2009)
"Not all patients with Parkinson's disease (PD) respond to levodopa and others develop dyskinesias."	1.32	Cost analysis of ropinirole versus levodopa in the treatment of Parkinson's disease. ( Einarson, TR; Iskedjian, M, 2003)
"Benserazide is commonly used for Parkinson's disease in combination with L-DOPA as a peripheral aromatic L-amino acid decarboxylase (AADC) inhibitor."	1.32	Effects of benserazide on L-DOPA-derived extracellular dopamine levels and aromatic L-amino acid decarboxylase activity in the striatum of 6-hydroxydopamine-lesioned rats. ( Arai, A; Kannari, K; Matsunaga, M; Shen, H; Yamato, H, 2003)
"Delusional jealousy in Parkinson's disease has rarely been reported in the scientific literature."	1.31	[A case of delusional jealousy in Parkinson disease ]. ( Brüne, M; Gerlach, G; Schröder, SG, 2001)
"Six patients with Parkinson's disease who had troublesome motor complications under levodopa/DCI and DA agonist combination therapy were compared in terms of the extent of motor complications and their satisfaction after changing their therapy from levodopa/DCI to levodopa without DCI."	1.31	[Benefit of L-DOPA-without-DCI (decarboxylase inhibitor) therapy on wearing-off phenomenon in advanced stages of Parkinson's disease patients]. ( Hironishi, M; Kondo, T; Miwa, H, 2002)
"Dysphagia is a frequent and potentially serious complication of Parkinson's disease (PD)."	1.30	Swallowing difficulty in Parkinson's disease. ( Chiang, JH; Fuh, JL; Lee, RC; Lin, CH; Liu, HC; Wang, PN; Wang, SJ, 1997)
" Daily levodopa dosage requirements decreased significantly."	1.30	Highlights of the North American and European experiences. ( Goetz, CG, 1998)
"Four of the patients had similar pharmacokinetic patterns for L-dopa and a significant (P < 0."	1.30	L-dopa pharmacokinetics studied with microdialysis in patients with Parkinson's disease and a history of malignant melanoma. ( Dizdar, N; Granérus, AK; Hannestad, U; Kågedal, B; Kullman, A; Ljungdahl, A; Olsson, JE, 1999)
" Two dosage strengths are available: 100 mg levodopa plus 25 mg benserazide and 50 mg levodopa plus 12."	1.29	[Benefits of a new galenic form of levodopa and benserazide in the treatment of patients with Parkinson disease]. ( Dessibourg, CA; Gachoud, JP, 1995)
"A 64-year-old man was diagnosed to have Parkinson's disease when aged 42 years and since then has been treated with levodopa and benserazide (up to 875 mg daily)."	1.29	[Bromocriptine-induced pleuropneumopathy]. ( Eberli, F; Greminger, P; Schmid, PA; Speich, R; Suter, T, 1994)
"Seven patients with idiopathic Parkinson's disease, aged 62 to 76 years, average duration of the disease approximately eleven years, suffering from severe hallucinosis and paranoid delusions of different degree, in whom conventional therapeutic strategies (administration of benzodiazepines and mild neuroleptics) had no antipsychotic effect, received clozapine, a non-classical highly potent neuroleptic, while blood count was strictly monitored."	1.29	Therapeutic effect of clozapine in psychotic decompensation in idiopathic Parkinson's disease. ( Helscher, RJ; Pinter, MM, 1993)
"Levodopa treatment might change the dopaminergic and serotoninergic neuronal systems, but not the noradrenergic or adrenergic neuronal systems, in CNS of PD patients."	1.29	Monoamines and their metabolites in plasma and lumbar cerebrospinal fluid of Chinese patients with Parkinson's disease. ( Cheng, FC; Chia, LG; Kuo, JS, 1993)
" Due to a lower bioavailability of the slow release formulation--the latter is based on the "hydrodynamically balanced system" (HBS)--, the patients remained initially on their time schedule of drug intake but received a higher dose of L-DOPA slow release compared to the preceding L-DOPA standard therapy."	1.29	[Effectiveness of slow release L-DOPA/benserazide in treatment of end-of-dose akinesia in Parkinson disease]. ( Eichhorn, TE; Kohnen, R; Oertel, WH; Poewe, W; Schrag, A; Selzer, R; Trenkwalder, C, 1995)
" As a consequence, levodopa dosage might be increased and the interdose interval progressively shortened."	1.29	Clinical implications of sustained dopaminergic stimulation. ( Barbato, L; Berardelli, A; Bonamartini, A; Manfredi, M; Patsalos, PN; Ruggieri, S; Stocchi, F, 1994)
"In patients with Parkinson's disease the levels of somatostatin-like immunoreactivity were lower than in controls (P less than ."	1.28	Somatostatin-like immunoreactivity in the cerebrospinal fluid of aged patients with Parkinson's disease. The effect of dopatherapy. ( Cramer, H; Kuntzmann, F; Masson, H; Popescu, I; Strubel, D, 1990)
"When benserazide was coadministered with RO 40-7592 (10 mg/kg) a dose-dependent decrease in striatal k3 was measured with an apparent ED50 of 3 mg/kg."	1.28	Central action of benserazide after COMT inhibition demonstrated in vivo by PET. ( Andersson, Y; Antoni, G; Bjurling, P; Hartvig, P; Långström, B; Tedroff, J, 1991)
"The current study on 36 patients with Parkinson's disease under long-term treatment with levodopa/dopadecarboxylase inhibitor showed, however, that the erythrocyte-COMT was unaffected by additional (-)-deprenyl medication."	1.28	(-)-Deprenyl treatment of patients with Parkinson's disease does not affect erythrocyte catechol-O-methyl transferase activity. ( Dettner, O; Gerlach, M; Kuhn, W; Przuntek, H; Russ, H, 1991)
" The negative aspects of Madopar HBS are a lower bioavailability that means a dosage increase and a longer latency for the therapeutic response in the morning."	1.28	Long-term treatment with Madopar HBS in parkinsonians with fluctuations. ( Aljanati, R; Buzó, R; Caamaño, JL; Chouza, C; De Medina, O; Fernandez, A; Plachín, V; Romero, S; Scaramelli, A, 1990)
"Fifty four patients with idiopathic Parkinson's disease receiving levodopa therapy were studied."	1.28	Severity of Parkinson's disease is a risk factor for peak-dose dyskinesia. ( Berger, HJ; Horstink, MW; Pasman, JW; van't Hof, MA; Zijlmans, JC, 1990)
"Selegiline was capable of enhancing the antiparkinsonian effect of the new formula of L-DOPA, while allowing a reduction of the doses administered."	1.28	Combination of selegiline and controlled release levodopa in the treatment of fluctuations of clinical disability in parkinsonian patients. ( Aljanati, R; Buzo, R; Caamaño, JL; Chouza, C; De Medina, O; Fernandez, A; Romero, S; Scaramelli, A, 1989)
" The optimal therapeutic dosage of Sinemet CR was equal to that of Madopar HBS but 12% higher than that of standard Madopar."	1.28	Treatment of early Parkinson's disease with controlled-release levodopa preparations. ( Rinne, JO; Rinne, UK, 1989)
" The effects of L-Dopa dosage adjustments after hospitalization were particularly considered."	1.28	[The problems of L-dopa therapy in the course of Parkinson syndrome]. ( Emskötter, T; Heidenreich, C; Lachenmayer, L, 1989)
" Plasma ALAAD 2 hours after dosing was normal in Groups I and II."	1.28	Induction of aromatic-L-amino acid decarboxylase by decarboxylase inhibitors in idiopathic parkinsonism. ( Boomsma, F; Hovestadt, A; Man in 't Veld, AJ; Meerwaldt, JD; Schalekamp, MA, 1989)
" The model is then used to optimize the dosage regimen for each patient individually (according to the clinical particularities and needs of each patient) with respect to an objective function which includes the symptoms dynamically and the total amount of levodopa which is to be administered."	1.28	Optimization of symptomatic therapy in Parkinson's disease. ( Albani, C; Hacisalihzade, SS; Mansour, M, 1989)
" Following effective stereotaxic surgery, drug therapy should be continued with reduced dosage of the drugs."	1.27	[Combined (surgical and drug) therapy of parkinsonism]. ( Iadgarov, IS; Kandel', EI, 1984)
"In the initial stage of Parkinson's disease deprenyl is only partially sufficient as monotherapy."	1.27	Clinical evaluation of deprenyl (selegiline) in the treatment of Parkinson's disease. ( Csanda, E; Tárczy, M, 1983)
"A 77-year-old man with Parkinson's disease of long standing, under treatment with L-DOPA and benserazide, was administered DL-threo-3, 4-dihydroxyphenylserine (DL-threo-DOPS), a precursor of norepinephrine, for 10 days."	1.27	Improvement in freezing phenomenon of Parkinson's disease after DL-threo-3, 4-dihydroxyphenylserine. ( Kuroda, H; Nukina, I; Ogawa, N; Ota, Z; Yamamoto, M, 1984)
"Benserazide was combined with carbidopa in 38 patients who were experiencing a diminished response to carbidopa, including 22 patients with diurnal oscillations in performance, "wearing off" or on-off phenomena."	1.27	Combined use of benserazide and carbidopa in Parkinson's disease. ( Goldstein, M; Gopinathan, G; Hiesiger, E; Lieberman, AN; Nelson, J; Neophytides, A; Walker, R, 1984)
"Four cases of dystonia occurring in two families are reported."	1.27	Dystonia--L-dopa responsive or juvenile parkinsonism? ( Rondot, P; Ziegler, M, 1983)
"A number of patients with Parkinson's disease complain of severe and distressing pain."	1.27	Painful Parkinson's disease. ( Koller, WC; Lang, AE; Marsden, CD; Quinn, NP, 1986)
"In addition the time from the onset of Parkinson's disease to significantly longer in the group of patients which were treated with Madopar and (-)deprenyl in combination."	1.27	Effect of (-)deprenyl in long-term treatment of Parkinson's disease. A 10-years experience. ( Birkmayer, GD; Birkmayer, W, 1986)
" In 13 patients a considerable diminution in nocturnal akinesia and in the frequency of waking up was reached with a mean dosage of 308 mg of Madopar HBS."	1.27	Madopar HBS in Parkinson patients with nocturnal akinesia. ( Jansen, EN; Meerwaldt, JD, 1988)
" At the end of the dosage adaptation phase (9 weeks) most patients improved; in patients with 'on-off' phenomenon, parkinsonism became less severe, on periods were longer, and fluctuations decrease; end-of-dose impairment resolved in 4 patients."	1.27	Substitution of standard Madopar by Madopar HBS in parkinsonians with fluctuations. ( Aljanati, R; Caamano, JL; Chouza, C; de Medina, O; Gonzales Panizza, V; Romero, S; Scarmelli, A, 1987)
" The dosage was adjusted until optimal response was obtained."	1.27	Madopar HBS: slow-release levodopa and benserazide in parkinsonian patients presenting marked fluctuations in symptoms on standard L-dopa treatment. ( Dupont, E; Hansen, E; Jensen, NO; Mikkelsen, B; Mikkelsen, BO, 1987)
" In all patients of the first group, after 3 months on stable 'optimal' dosage schedule, the previous L-dopa treatment was abruptly replaced, dose for dose, from one day to another by Madopar HBS, a new controlled-release form of Madopar."	1.27	Therapeutic value of Madopar HBS: judgment after 2 years experience. ( Siegfried, J, 1987)
" In nine subjects who completed the trial, the clinical response, occurrence of dyskinesias and of nausea and vomiting, were similar with both treatments, although peak plasma levodopa concentration and levodopa bioavailability were greater on levodopa-domperidone than on levodopa-carbidopa."	1.27	Comparison of levodopa with carbidopa, and levodopa with domperidone in Parkinson's disease. ( Langdon, N; Malcolm, PN; Parkes, JD, 1986)
"Levodopa treatment alleviated the parkinsonian symptoms to a considerable degree and substantially improved the quality of life of the parkinsonian patients."	1.26	Long-term responses of Parkinson's disease to levodopa therapy. ( Marttila, R; Rinne, UK; Siirtola, T; Sonninen, V, 1980)
"Levodopa 40 mg was taken at intervals of half to two and a half hours, usually with benserazide 10 mg but alone in the late morning and evening."	1.26	Improved control of brittle Parkinsonism by separate administration of levodopa and benserazide. ( Dean, BC; McLellan, DL, 1982)
" PRL increase after benserazide was compared with PRL response after carbidopa at the same dosage in untreated parkinsonian patients."	1.26	Prolactin response to acute administration of different L-dopa plus decarboxylase inhibitors in Parkinson's disease. ( Agnoli, A; Baldassarre, M; D'Urso, R; De Giorgio, G; Falaschi, P; Rocco, A; Ruggieri, S, 1982)
"CDP-choline treatment showed a significant improvement of rigidity and bradykinesia and a less important amelioration of tremor."	1.26	New strategies in the management of Parkinson's disease: a biological approach using a phospholipid precursor (CDP-choline). ( Agnoli, A; Bruno, G; Denaro, A; Ruggieri, S, 1982)
" Reduction of levodopa dosage to one sixth with the aid of a peripheral decarboxylase inhibitor (benserazide) largely eliminated autoimmune haemolysis while maintaining adequate control of neurologic symptoms."	1.26	Dose-related levodopa-induced haemolytic anaemia. ( Enström, MS; Liedén, G; Linström, FD, 1977)
"Twenty-six patients affected by Parkinson's disease were treated with a 2-Br-alpha-ergocriptine (CB 154): 14 cases were given CB 154 alone, and 12 were given CB 154 along with L-dopa plus benserazide (Madopar)."	1.26	Bromocriptine alone or associated with L-dopa plus benserazide in Parkinson's disease. ( Caraceni, TA; Celano, I; Girotti, F; Parati, E, 1977)
"Levodopa treatment, alone or in combination with two different dopa-decarboxylase inhibitors, benserazide and carbidopa, does not modify the renin response to posture or to frusemide."	1.26	Effects of levodopa alone and in combination with dopa-decarboxylase inhibitors on plasma renin activity in patients with Parkinson's disease. ( Dessi'-Fulgheri, P; Glorioso, N; Monaco, F; Rappelli, A; Tedde, R, 1978)
"A patient with Parkinson's disease, in whom polycythemia vera was known to be present for several years prior to the onset of parkinsonian symptoms, received treatment with a preparation consisting of L-dopa plus a decarboxylase inhibitor (Madopar)."	1.26	Effect of L-dopa on polycythemia. ( Herishanu, Y; Rosenberg, P, 1977)
"Since L-dopa in combination with a decarboxylase inhibitor is currently the most effective therapy available for treatment of Parkinson's disease, the authors compare the actual causes of death in a large series of treated Parkinson patients with a normal population and with previous studies."	1.26	Mortality among Parkinson patients treated with L-dopa combined with a decarboxylase inhibitor. ( Siegfried, J; Zumstein, H, 1976)
" A reduced mean L-Dopa dosage was ruled out as the cause of this deterioration."	1.26	Study of deterioration in long-term treatment of parkinsonism with L-dopa plus decarboxylase inhibitor. ( Bass-Verrey, F; Ludin, HP, 1976)
" The adverse effect reappeared in a more severe and prolonged form when she was treated one year later with levodopa in combination with the peripheral decarboxylase inhibitor Ro-4-4602."	1.26	Prolonged symptoms of brain dysfunction--adverse effect of levodopa. ( Anggård, E; Samuelsson, K, 1976)
"Eighty-one Parkinsonic patients were treated with L-dopa alone and/or combined with Ro4-4602, during 27 to 60 months."	1.26	[5 years of experience in the treatment of parkinsonism with L-dopa and its combination with Ro4-4602]. ( Chouza, C; Gomensoro, JB; Romero, S, 1976)
"Levodopa induced an increase of about 400 fold in urinary DA; DOPAC was increased about 300 fold, 3-MT only about 70 fold, but HVA about 300 fold."	1.25	Urinary excretion of monoamines and their metabolites in patients with Parkinson's disease. Response to long-term treatment with levodopa alone or in combination with a dopa decarboxylase inhibitor and clinical correlations. ( Rinne, UK; Siirtola, T; Sonninen, V, 1975)
" Observations were repeated with varying dosage patterns, showing variations but no substantial changes or disappearance of the symptoms described."	1.25	[Long-term syndrome in the treatment of parkinsonism with L-dopa]. ( Chouza, C; Gomensoro, JB; Romero, S, 1975)

Research

Studies (340)

Authors

Clinical Trials (6)

Trial Overview

Trial Outcomes

306A Efficacy: Change in Orthostatic Hypotension Questionnaire Score (OHQ)

Timeframe	Studies, this research(%)	All Research%
pre-1990	168 (49.41)	18.7374
1990's	71 (20.88)	18.2507
2000's	34 (10.00)	29.6817
2010's	59 (17.35)	24.3611
2020's	8 (2.35)	2.80

Authors	Studies
Daidone, F	1
Montioli, R	1
Paiardini, A	1
Cellini, B	1
Macchiarulo, A	1
Giardina, G	1
Bossa, F	1
Borri Voltattorni, C	1
Banerjee, A	1
Patil, S	1
Pawar, MY	1
Gullapalli, S	1
Gupta, PK	1
Gandhi, MN	1
Bhateja, DK	1
Bajpai, M	1
Sangana, RR	1
Gudi, GS	1
Khairatkar-Joshi, N	1
Gharat, LA	1
Baba, Y	1
Futamura, A	1
Kinno, R	1
Nomoto, S	1
Takahashi, S	1
Yasumoto, T	1
Osakabe, Y	1
Shoji, D	1
Nabeshima, Y	1
Su, D	1
Su, Y	1
Xu, B	1
Chhetri, JK	1
Chan, P	3
Murakami, Y	1
Nishijima, H	1
Nakamura, T	3
Furukawa, T	1
Kinoshita, I	1
Kon, T	1
Suzuki, C	1
Tomiyama, M	1
Yang, Y	1
Gao, F	1
Gao, L	1
Miao, J	1
van Nuland, AJ	1
Helmich, RC	2
Dirkx, MF	2
Zach, H	2
Toni, I	1
Cools, R	1
den Ouden, HEM	1
Santos, MEHP	1
Olops, L	1
Vendrame, F	1
Tavares, AHJ	1
Leonardo, DP	1
de Azevedo, PC	1
Piovesana, LG	1
Costa, FF	1
Fertrin, KY	1
Ong, TL	1
Dal, S	1
Martin, AJ	1
Chang, FC	1
Williams, LJ	1
Babu, S	1
Mahant, N	1
Morales-Briceno, H	1
Fletcher, N	1
Nankervis, J	1
Robbie, M	1
Fung, VSC	1
Jiang, DQ	1
Zang, QM	1
Jiang, LL	1
Wang, Y	3
Li, MX	1
Qiao, JY	1
Seiffert, P	1
Derejczyk, J	1
Kawa, J	1
Marcisz, C	1
Czernek, M	1
Szymszal, J	1
Kapko, W	1
Bugdol, M	1
Torbus, A	1
Stępień-Wyrobiec, O	1
Cilia, R	1
Laguna, J	1
Cassani, E	1
Cereda, E	1
Pozzi, NG	3
Isaias, IU	3
Contin, M	5
Barichella, M	1
Pezzoli, G	5
Yoosefian, M	1
Rahmanifar, E	1
Etminan, N	1
Lee, HD	1
Chang, MC	1
Bloem, BR	1
Hallett, M	2
Turco, F	1
Canessa, A	2
Olivieri, C	1
Palmisano, C	2
Arnulfo, G	1
Marotta, G	1
Volkmann, J	2
Chandel, TI	1
Zaidi, N	1
Zaman, M	1
Jahan, I	1
Masroor, A	1
Siddique, IA	1
Nayeem, SM	1
Ali, M	1
Uversky, VN	1
Khan, RH	1
Brandt, G	1
Leporini, A	1
Maltese, V	1
Frigo, CA	1
Torti, M	1
Alessandroni, J	1
Bravi, D	1
Casali, M	1
Grassini, P	1
Fossati, C	1
Ialongo, C	1
Onofrj, M	1
Radicati, FG	1
Vacca, L	1
Bonassi, S	1
Stocchi, F	6
Gasser, UE	3
Fischer, A	1
Timmermans, JP	1
Arnet, I	1
Zhang, J	3
Ma, YZ	1
Shen, XM	1
Lopez, S	1
Bonito-Oliva, A	1
Pallottino, S	1
Acher, F	1
Fisone, G	1
Almeida, KJ	1
de Oliveira Filho, MC	1
Lopes Nery, PC	1
Guimarães Silva, JS	1
Campos Sousa, RN	1
Aquino, CC	1
Celso de Castro, P	1
Doná, F	1
Medeiros, L	1
Silva, SM	1
Borges, V	1
Ferraz, HB	1
Porras, G	1
De Deurwaerdere, P	1
Li, Q	1
Marti, M	2
Morgenstern, R	1
Sohr, R	1
Bezard, E	1
Morari, M	2
Meissner, WG	1
Hattori, N	1
Solís, O	1
Espadas, I	1
Del-Bel, EA	1
Moratalla, R	1
Xie, CL	1
Wang, WW	1
Zhang, SF	1
Yuan, ML	1
Che, JY	1
Gan, J	1
Song, L	1
Yuan, WE	1
Liu, ZG	1
Ferreira, JJ	3
Rocha, JF	3
Falcão, A	2
Santos, A	2
Pinto, R	2
Nunes, T	3
Soares-da-Silva, P	4
Alirezaei, M	1
Khoshdel, Z	1
Dezfoulian, O	1
Rashidipour, M	1
Taghadosi, V	1
Gellhaar, S	1
Marcellino, D	1
Abrams, MB	1
Galter, D	1
Epprecht, L	1
Schreglmann, SR	1
Goetze, O	1
Woitalla, D	3
Baumann, CR	1
Waldvogel, D	1
Shan, L	1
Diaz, O	1
Zhang, Y	1
Ladenheim, B	1
Cadet, JL	1
Chiang, YH	1
Olson, L	1
Hoffer, BJ	1
Bäckman, CM	1
Pan, X	1
Chen, C	1
Huang, J	1
Wei, H	1
Fan, Q	1
Song, JH	1
Zhou, PY	1
Cao, ZH	1
Ding, ZG	1
Chen, HX	1
Zhang, GB	1
Michel, A	1
Downey, P	1
Van Damme, X	1
De Wolf, C	1
Schwarting, R	1
Scheller, D	1
Kuoppamäki, M	2
Leinonen, M	2
Poewe, W	6
Wu, T	1
Feng, T	2
Hou, Y	2
Calandra-Buonaura, G	1
Doria, A	1
Lopane, G	1
Guaraldi, P	1
Capellari, S	1
Martinelli, P	4
Cortelli, P	1
Guo, Z	1
Xu, S	2
Du, N	1
Liu, J	1
Huang, Y	2
Han, M	1
Bang, JI	1
Jung, IS	1
Song, YS	1
Park, HS	1
Moon, BS	1
Lee, BC	1
Kim, SE	1
Almeida, L	2
Gonzalez-Maldonado, R	1
Gonzalez-Redondo, R	1
Di Caudo, C	1
Guo, G	1
Cao, LD	1
Wu, QY	1
Geng, X	1
Wang, X	2
Xie, J	1
Zhang, X	1
Lei, C	1
Li, M	3
Han, H	1
Yao, X	1
Zhang, Q	1
Wang, M	1
Adams, F	1
Boschmann, M	1
Lobsien, E	1
Kupsch, A	1
Lipp, A	1
Franke, G	1
Leisse, MC	1
Janke, J	1
Gottschalk, S	1
Spranger, J	1
Jordan, J	1
Fung, VS	1
Herawati, L	1
Wan, Y	1
Li, W	1
Lu, L	1
Shi, W	1
Ren, XM	1
Cannas, A	2
Solla, P	2
Floris, G	2
Tacconi, P	2
Serra, A	1
Piga, M	1
Marrosu, F	1
Marrosu, MG	1
Wang, HB	1
Hsu, CH	1
Jiang, X	1
Zhuo, Y	1
Tang, A	1
Wik, G	1
Eggert, K	2
Skogar, O	1
Amar, K	1
Luotonen, L	1
Nissinen, H	1
Oertel, W	1
Adamiak, U	1
Kaldonska, M	1
Klodowska-Duda, G	1
Wyska, E	1
Safranow, K	1
Bialecka, M	1
Gawronska-Szklarz, B	1
Kobylecki, C	1
Cenci, MA	1
Crossman, AR	1
Ravenscroft, P	1
Müller, T	6
Muhlack, S	5
Ries, V	1
Selzer, R	2
Eichhorn, T	1
Oertel, WH	3
Stefanis, N	1
Bozi, M	1
Christodoulou, C	1
Douzenis, A	1
Gasparinatos, G	1
Stamboulis, E	1
Stefanis, C	1
Stefanis, L	1
Rascol, O	2
Sampaio, C	1
Prakash, KM	1
Kek, PC	1
Tani, Y	1
Ogata, A	1
Koyama, M	1
Inoue, T	1
Gil, SJ	1
Park, CH	1
Lee, JE	1
Minn, YK	1
Koh, HC	1
Dick, OE	1
Romanov, SP	1
Nozdrachev, AD	1
Hashim, HZ	1
Wan Musa, WR	1
Ngiu, CS	1
Wan Yahya, WN	1
Tan, HJ	1
Ibrahim, N	1
Adam, JJ	1
van Houdt, H	1
Scholtissen, B	1
Visser-Vandewalle, V	1
Winogrodzka, A	1
Duits, A	1
Geiser, E	1
Kaelin-Lang, A	1
Ishihara, A	1
Miyachi, T	1
Ohtsuki, T	1
Kimura, Y	1
Kihira, K	1
Yamawaki, T	1
Matsumoto, M	1
Yang, MH	2
Li, SD	1
Liu, Y	2
Costa, C	1
Sgobio, C	1
Siliquini, S	1
Tozzi, A	1
Tantucci, M	1
Ghiglieri, V	1
Di Filippo, M	1
Pendolino, V	1
de Iure, A	1
Spillantini, MG	1
Latagliata, EC	1
Pascucci, T	1
Puglisi-Allegra, S	1
Gardoni, F	1
Di Luca, M	1
Picconi, B	1
Calabresi, P	1
Gerlach, M	2
Halley, P	1
Riederer, P	6
van den Buuse, M	1
El Otmani, H	1
Moutaouakil, F	1
Fadel, H	1
Slassi, I	1
Zavala, JA	1
Munhoz, RP	1
Teive, HA	1
Grandas, FJ	1
Sesar-Ignacio, Á	1
Iskedjian, M	1
Einarson, TR	1
Shen, H	1
Kannari, K	1
Yamato, H	1
Arai, A	1
Matsunaga, M	1
Scaglione, C	1
Riva, R	3
Albani, F	2
Baruzzi, A	3
Yoshida, T	1
Kono, I	1
Yoshikawa, K	1
Hashimoto, H	1
Harada, H	1
Nakagawa, M	1
Welnic, J	3
Twiehaus, S	1
Przuntek, H	6
Mochi, M	1
Ludin, HP	3
St-Hilaire, M	1
Bourhis, E	1
Lévesque, D	1
Rouillard, C	1
Fleming, SM	1
Salcedo, J	1
Hutson, CB	1
Rockenstein, E	1
Masliah, E	1
Levine, MS	1
Chesselet, MF	1
Chen, XH	1
Li, Y	1
Kui, Y	1
Lian, XF	1
Luo, XD	1
Pinessi, L	1
Sabbatini, F	1
De Mattei, M	1
Gentile, S	1
Fischer, PA	4
Majer, M	1
Welzel, D	2
Kandel', EI	1
Iadgarov, IS	1
Birkmayer, W	8
Birkmayer, G	1
Lechner, H	1
Fekete, M	1
Tárczy, M	4
Bihari, K	1
Katona, G	2
Csanda, E	3
Takáts, A	2
Mogyorós, I	1
Köves, A	1
Gerstenbrand, F	1
Ransmayr, G	2
Ogawa, N	1
Kuroda, H	1
Yamamoto, M	2
Nukina, I	1
Ota, Z	1
Da Prada, M	2
Keller, HH	1
Pieri, L	1
Kettler, R	1
Haefely, WE	1
Martinez-Campos, A	3
Giovannini, P	4
Cocchi, D	2
Zanardi, P	1
Parati, EA	1
Caraceni, T	4
Müller, EE	3
Lieberman, AN	2
Goldstein, M	2
Gopinathan, G	2
Neophytides, A	1
Hiesiger, E	1
Walker, R	1
Nelson, J	1
Rondot, P	6
Ziegler, M	3
Baldassarre, G	1
Fazio, B	1
Vogel, HP	2
Schiffter, R	1

Trial	Phase	Enrollment	Study Type	Start Date	Status
Mucuna Pruriens Therapy in Parkinson's Disease: a Double-blind, Placebo-controlled, Randomized, Crossover Study.[NCT02680977]	Phase 2	18 participants (Actual)	Interventional	2016-02-29	Completed
Comparison of Blood Dopamine Levels in Idiopathic Parkinson's Patients Receiving Levodopa Carbidopa Entacapone or Levodopa Benserazide[NCT06115538]	Phase 4	96 participants (Anticipated)	Interventional	2023-10-01	Enrolling by invitation
Orthostatic Dysregulation and Associated Gastrointestinal Dysfunction in Parkinson's Disease - Evolution A Monocentric Study to Investigate the Development of Symptoms of Autonomic Dysregulation in Parkinson's Disease[NCT01518751]		27 participants (Actual)	Observational	2011-12-31	Completed
A Multi-center, Double-blind, Randomized, Parallel-Group, Placebo-Controlled Study to Assess the Clinical Effect of Droxidopa in the Treatment of Symptomatic Neurogenic Orthostatic Hypotension in Patients With Parkinson's Disease[NCT01176240]	Phase 3	225 participants (Actual)	Interventional	2010-06-30	Completed
The Effects of Supplementing Tyrosine on Blood Pressure in Parkinson's Disease[NCT01676103]	Phase 1/Phase 2	40 participants (Actual)	Interventional	2012-09-30	Completed
The Influence of Sensory Stimuli on Gait Imagery in Patients With Freezing of Gait[NCT01071590]		45 participants (Actual)	Observational	2010-02-01	Completed
[information is prepared from clinicaltrials.gov, extracted Sep-2024]

"The primary efficacy endpoint for 306A is the relative mean change in Orthostatic Hypotension Questionnaire (OHQ) composite score from baseline to end of study. The OHQ is the average of two sub-scales, the Orthostatic Hypotension Symptom Assessment Scale (OHSA) and the Orthostatic Hypotension Daily Activities Scale (OHDAS). Each asks the patient to rate their symptoms or disease impact over the past week. The OHSA sub-scale is the average of six items: 1) Dizziness, lightheadedness, feeling faint or feeling like you might black out; 2) Problems with vision; 3) Weakness; 4) Fatigue; 5) Trouble concentrating; and 6) Head/neck discomfort. The OHDAS sub-scale is the average of four items: 1) Standing for a short time; 2) Standing for a long time; 3) Walking for a short time; and 4) Walking for a long time. Each item is scored on a Likert scale from 0 to 10, with 10 being the most severe.~For the change from baseline, negative numbers represent improvement from baseline in OHQ score." (NCT01176240)
Timeframe: Baseline, Week 8

306A Efficacy: Patient Reported Falls

Intervention	units on a scale (Mean)
Droxidopa	-2.2
Placebo	-2.1

The total number of patient reported falls during the 8 week treatment period (NCT01176240)
Timeframe: Baseline, Week 8

306B Efficacy: Change in Dizziness/Lightheadedness/Feeling Faint/Feeling Like You Might Black Out (OHSA Item 1)

Intervention	total falls per group (Number)
Droxidopa	79
Placebo	192

OHSA item 1 scale range: 0 (none) -10 (worst), likert scale. Change: score at Week 1 minus score at baseline. A negative score indicates an improvement in symptoms during the double-blind randomized phase relative to value at baseline. (NCT01176240)
Timeframe: Baseline, Week1

306B Efficacy: Change in OHSA Item 1 From Baseline to Week 2 (Visit 5)

Intervention	units on a scale (Mean)
Droxidopa	-2.3
Placebo	-1.3

OHSA item 1 scale range: 0 (none) -10 (worst), likert scale. Change: score at Week 2 minus score at baseline. A negative score indicates an improvement in symptoms during the double-blind randomized phase relative to value at baseline. (NCT01176240)
Timeframe: Baseline, Week2

306B Efficacy: Change in OHSA Item 1 From Baseline to Week 4 (Visit 6)

Intervention	units on a scale (Mean)
Droxidopa	-1.9
Placebo	-1.6

OHSA item 1 scale range: 0 (none) -10 (worst), likert scale. Change: score at Week 4 minus score at baseline. A negative score indicates an improvement in symptoms during the double-blind randomized phase relative to value at baseline. (NCT01176240)
Timeframe: Baseline, Week4

306B Efficacy: Change in OHSA Item 1 From Baseline to Week 8 (Visit 7)

Intervention	units on a scale (Mean)
Droxidopa	-2.0
Placebo	-1.5

OHSA item 1 scale range: 0 (none) -10 (worst), likert scale. Change: score at Week 8 minus score at baseline. A negative score indicates an improvement in symptoms during the double-blind randomized phase relative to value at baseline. (NCT01176240)
Timeframe: Baseline, Week 8

306B Efficacy: Change in Orthostatic Hypotension Questionnaire Score (OHQ)

Intervention	units on a scale (Mean)
Droxidopa	-2.1
Placebo	-1.5

"The relative mean change in Orthostatic Hypotension Questionnaire (OHQ) composite score from baseline to end of study. The OHQ is the average of two sub-scales, the Orthostatic Hypotension Symptom Assessment Scale (OHSA) and the Orthostatic Hypotension Daily Activities Scale (OHDAS). Each asks the patient to rate their symptoms or disease impact over the past week. The OHSA sub-scale is the average of six items: 1) Dizziness, lightheadedness, feeling faint or feeling like you might black out; 2) Problems with vision; 3) Weakness; 4) Fatigue; 5) Trouble concentrating; and 6) Head/neck discomfort. The OHDAS sub-scale is the average of four items: 1) Standing for a short time; 2) Standing for a long time; 3) Walking for a short time; and 4) Walking for a long time. Each item is scored on a Likert scale from 0 to 10, with 10 being the most severe.~For the change from baseline, negative numbers represent improvement from baseline in OHQ score." (NCT01176240)
Timeframe: Baseline, Week 8

306B Efficacy: Change in Systolic Blood Pressure (SBP) Measurements Post Standing From Baseline to Week 1

Intervention	units on a scale (Mean)
Droxidopa	-2.2
Placebo	-2.0

Measure: Lowest standing systolic blood pressure reading of immediately post standing and 3 minutes post standing. Change: standing systolic blood pressure at Week 1 (Visit 4) minus standing systolic blood pressure at baseline. A positive score indicates an improvement in standing systolic blood pressure during the double-blind randomized phase relative to value at baseline. (NCT01176240)
Timeframe: Baseline, Week 1

306B Efficacy: Rate of Patient Reported Falls

Intervention	mmHg (Mean)
Droxidopa	6.4
Placebo	0.7

The average number of patient reported falls per week. (NCT01176240)
Timeframe: up to 10 weeks

Study 306A: Change in Dizziness/Lightheadedness/Feeling Faint/Feeling Like You Might Black Out (OHSA Item 1) From Baseline to Week 1

Intervention	falls per week (Mean)
Droxidopa	0.4
Placebo	2.0

OHSA item 1 scale range: 0 (none) -10 (worst), likert scale. Change: score at Week 1 minus score at baseline. A negative score indicates improvement in symptoms during the double-blind randomized phase relative to value at baseline. (NCT01176240)
Timeframe: Baseline, Week 1

Article	Year
Comparison of pramipexole and levodopa/benserazide combination therapy versus levodopa/benserazide monotherapy in the treatment of Parkinson's disease: a systematic review and meta-analysis. Naunyn-Schmiedeberg's archives of pharmacology, 2021, Volume: 394, Issue:9 Topics: Antiparkinson Agents; Benserazide; Drug Combinations; Drug Therapy, Combination; Humans; Levodopa; P	2021
[Programs for continuing medical education: a session: 4. The pathogenesis and update for the treatments of Parkinson's disease]. Nihon Naika Gakkai zasshi. The Journal of the Japanese Society of Internal Medicine, 2014, Mar-10, Volume: 103, Issue:3 Topics: Benserazide; Benzothiazoles; Catechols; Circadian Rhythm; Dementia; Dopamine Agonists; Drug Combinat	2014
[Subcutaneous continuous apomorphine infusion: treatment initiation and follow up]. Revista de neurologia, 2012, Volume: 55 Suppl 1 Topics: Aftercare; Ambulatory Care; Antiparkinson Agents; Apomorphine; Benserazide; Carbidopa; Caregivers; D	2012
[Idiopathic Parkinson's disease: practical hints for the treatment]. Praxis, 2005, Jul-27, Volume: 94, Issue:30-31 Topics: Adult; Aged; Antidepressive Agents; Antiparkinson Agents; Antipsychotic Agents; Benserazide; Choline	2005
The pharmacology of Parkinson's disease: basic aspects and recent advances. Experientia, 1984, Nov-15, Volume: 40, Issue:11 Topics: Animals; Antiparkinson Agents; Aromatic Amino Acid Decarboxylase Inhibitors; Benserazide; Brain; Bro	1984
Growth hormone secretion in neurological disorders. Advances in biochemical psychopharmacology, 1981, Volume: 28 Topics: Benserazide; Disease Models, Animal; Dopamine; Growth Hormone; Humans; Huntington Disease; Levodopa;	1981
[Antiparkinsonian drugs (author's transl)]. No to shinkei = Brain and nerve, 1980, Volume: 32, Issue:8 Topics: Amantadine; Antiparkinson Agents; Benserazide; Dopamine; Humans; Levodopa; Monoamine Oxidase Inhibit	1980
[Vascular hemi-parkinson disease]. Revue neurologique, 1993, Volume: 149, Issue:10 Topics: Aged; Aspirin; Benserazide; Brain Ischemia; Drug Therapy, Combination; Female; Functional Laterality	1993
The syndrome of gait ignition failure: a report of six cases. Movement disorders : official journal of the Movement Disorder Society, 1993, Volume: 8, Issue:3 Topics: Aged; Benserazide; Brain; Carbidopa; Diagnosis, Differential; Drug Therapy, Combination; Female; Gai	1993
Pregnancy in Parkinson's disease: a review of the literature and a case report. Movement disorders : official journal of the Movement Disorder Society, 1998, Volume: 13, Issue:1 Topics: Abnormalities, Drug-Induced; Adjuvants, Pharmaceutic; Adult; Amantadine; Animals; Antiparkinson Agen	1998
[Parkinson's disease and pregnancy: case report and literature review]. Journal de gynecologie, obstetrique et biologie de la reproduction, 2000, Volume: 29, Issue:5 Topics: Adult; Antiparkinson Agents; Benserazide; Drug Combinations; Female; Humans; Infant, Newborn; Levodo	2000
Recent advances in research on Parkinsonism. Acta neurologica Scandinavica. Supplementum, 1978, Volume: 67 Topics: Acetylcholinesterase; Adult; Apomorphine; Benserazide; Brain; Bromocriptine; Carbidopa; Dopa Decarbo	1978
Levodopa. Annals of internal medicine, 1975, Volume: 83, Issue:5 Topics: Benserazide; Drug Interactions; Hepatic Encephalopathy; Humans; Huntington Disease; Levodopa; Melano	1975
Levodopa and decarboxylase inhibitors: a review of their clinical pharmacology and use in the treatment of parkinsonism. Drugs, 1976, Volume: 11, Issue:5 Topics: Benserazide; Binding Sites; Carbidopa; Carboxy-Lyases; Drug Interactions; Humans; Hydrazines; Kineti	1976
New approaches to the treatment of age-related brain disorders. The Canadian journal of neurological sciences. Le journal canadien des sciences neurologiques, 1991, Volume: 18, Issue:3 Suppl Topics: Aging; Alzheimer Disease; Benserazide; Benzophenones; Catechol O-Methyltransferase Inhibitors; Drug	1991
Levodopa treatment of Parkinson's syndrome: past and future. Advances in neurology, 1990, Volume: 53 Topics: Benserazide; Brain; Carboxy-Lyases; Drug Therapy, Combination; Forecasting; Humans; Levodopa; Parkin	1990
R-(-)-deprenyl and parkinsonism. Journal of neural transmission. Supplementum, 1987, Volume: 25 Topics: 1-Methyl-4-phenyl-1,2,3,6-tetrahydropyridine; Benserazide; Clorgyline; Dopamine; Drug Therapy, Combi	1987
[Influencing of Parkinson's syndrome via intervention in the dopamine metabolism]. Nederlands tijdschrift voor geneeskunde, 1973, Feb-24, Volume: 117, Issue:8 Topics: Acetylcholine; Action Potentials; Benserazide; Dihydroxyphenylalanine; Dopamine; Drug Combinations;	1973
[Decarboxylase inhibitor given in combination with l-dopa. A new therapeutic principal in parkinsonism]. Tidsskrift for den Norske laegeforening : tidsskrift for praktisk medicin, ny raekke, 1973, Oct-10, Volume: 93, Issue:28 Topics: Administration, Oral; Animals; Benserazide; Dihydroxyphenylalanine; Drug Therapy, Combination; Human	1973

Article	Year
Age as a risk factor for orthostatic hypotension induced by the levodopa challenge test in patients with Parkinson's disease: Results from a single-center trial. Medicine, 2023, Mar-03, Volume: 102, Issue:9 Topics: Benserazide; Humans; Hypotension, Orthostatic; Levodopa; Parkinson Disease; Risk Factors	2023
Neurology, 2017, Aug-01, Volume: 89, Issue:5 Topics: Antiparkinson Agents; Benserazide; Blood Pressure; Cross-Over Studies; Dose-Response Relationship, D	2017
Clinical and pharmacokinetics equivalence of multiple doses of levodopa benserazide generic formulation vs the originator (Madopar). British journal of clinical pharmacology, 2019, Volume: 85, Issue:11 Topics: Adult; Aged; Benserazide; Cross-Over Studies; Dopamine Agents; Double-Blind Method; Drug Combination	2019
Evaluation on the efficacy and safety of Chinese herbal medication Xifeng Dingchan Pill in treating Parkinson's disease: study protocol of a multicenter, open-label, randomized active-controlled trial. Journal of integrative medicine, 2013, Volume: 11, Issue:4 Topics: Benserazide; Data Interpretation, Statistical; Drug Combinations; Drugs, Chinese Herbal; Humans; Lev	2013
Effect of opicapone on levodopa pharmacokinetics, catechol-O-methyltransferase activity and motor fluctuations in patients with Parkinson's disease. European journal of neurology, 2015, Volume: 22, Issue:5 Topics: Aged; Aged, 80 and over; Antiparkinson Agents; Benserazide; Carbidopa; Catechol O-Methyltransferase;	2015
Unchanged gastric emptying and visceral perception in early Parkinson's disease after a high caloric test meal. Journal of neurology, 2015, Volume: 262, Issue:8 Topics: Adult; Aged; Appetite; Benserazide; Breath Tests; Caprylates; Dopamine Agents; Drug Combinations; Ga	2015
Rhythmic auditory stimulation with visual stimuli on motor and balance function of patients with Parkinson's disease. European review for medical and pharmacological sciences, 2015, Volume: 19, Issue:11 Topics: Acoustic Stimulation; Aged; Benserazide; Benzothiazoles; Catechols; Dose-Response Relationship, Drug	2015
Efficacy and safety of entacapone in levodopa/carbidopa versus levodopa/benserazide treated Parkinson's disease patients with wearing-off. Journal of neural transmission (Vienna, Austria : 1996), 2015, Volume: 122, Issue:12 Topics: Antiparkinson Agents; Benserazide; Carbidopa; Catechol O-Methyltransferase Inhibitors; Catechols; Da	2015
Neural correlates underlying micrographia in Parkinson's disease. Brain : a journal of neurology, 2016, Volume: 139, Issue:Pt 1 Topics: Aged; Attention; Basal Ganglia; Benserazide; Brain Mapping; Case-Control Studies; Cerebellum; Drug C	2016
Effect of 3 Single-Dose Regimens of Opicapone on Levodopa Pharmacokinetics, Catechol-O-Methyltransferase Activity and Motor Response in Patients With Parkinson Disease. Clinical pharmacology in drug development, 2016, Volume: 5, Issue:3 Topics: Adult; Aged; Antiparkinson Agents; Benserazide; Carbidopa; Catechol O-Methyltransferase; Catechol O-	2016
Quality of life in early Parkinson's disease treated with levodopa/carbidopa/entacapone. Movement disorders : official journal of the Movement Disorder Society, 2009, Jan-15, Volume: 24, Issue:1 Topics: Aged; Antiparkinson Agents; Benserazide; Carbidopa; Catechol O-Methyltransferase Inhibitors; Catecho	2009
Fifty cases of Parkinson's disease treated by acupuncture combined with madopar. Journal of traditional Chinese medicine = Chung i tsa chih ying wen pan, 2008, Volume: 28, Issue:4 Topics: Acupuncture Therapy; Aged; Benserazide; Combined Modality Therapy; Drug Combinations; Female; Humans	2008
Direct switch from levodopa/benserazide or levodopa/carbidopa to levodopa/carbidopa/entacapone in Parkinson's disease patients with wearing-off: efficacy, safety and feasibility--an open-label, 6-week study. Journal of neural transmission (Vienna, Austria : 1996), 2010, Volume: 117, Issue:3 Topics: Aged; Antiparkinson Agents; Benserazide; Carbidopa; Catechols; Drug-Related Side Effects and Adverse	2010
Pharmacokinetic-pharmacodynamic modeling of levodopa in patients with advanced Parkinson disease. Clinical neuropharmacology, 2010, Volume: 33, Issue:3 Topics: Age of Onset; Aged; Antiparkinson Agents; Aromatic Amino Acid Decarboxylase Inhibitors; Benserazide;	2010
Effect of exercise on reactivity and motor behaviour in patients with Parkinson's disease. Journal of neurology, neurosurgery, and psychiatry, 2010, Volume: 81, Issue:7 Topics: Aged; Antiparkinson Agents; Attention; Basal Ganglia; Benserazide; Dopamine; Dopamine Agents; Execut	2010
Replacing a dopamine agonist by the COMT-inhibitor tolcapone as an adjunct to L-dopa in the treatment of Parkinson's disease: a randomized, multicenter, open-label, parallel-group study. Clinical neuropharmacology, 2010, Volume: 33, Issue:3 Topics: Aged; Ambulatory Care Facilities; Aromatic Amino Acid Decarboxylase Inhibitors; Benserazide; Benzoph	2010
A double-blind, randomized, placebo and active-controlled study of nebicapone for the treatment of motor fluctuations in Parkinson's disease. CNS neuroscience & therapeutics, 2010, Volume: 16, Issue:6 Topics: Acetophenones; Adult; Aged; Aged, 80 and over; Antiparkinson Agents; Benserazide; Carbidopa; Catecho	2010
[Effects of bushenhuoxue granules on sleep quality in Parkinson's patients]. Zhong yao cai = Zhongyaocai = Journal of Chinese medicinal materials, 2011, Volume: 34, Issue:9 Topics: Aged; Aged, 80 and over; Benserazide; Double-Blind Method; Drug Combinations; Drugs, Chinese Herbal;	2011
[Effects of "attenuation and synergia" for Bushenhuoxue Granules on Parkinson's patients]. Zhong yao cai = Zhongyaocai = Journal of Chinese medicinal materials, 2012, Volume: 35, Issue:3 Topics: Administration, Oral; Aged; Aged, 80 and over; Antiparkinson Agents; Benserazide; Constipation; Doub	2012
Chronic levodopa intake increases levodopa plasma bioavailability in patients with Parkinson's disease. Neuroscience letters, 2004, Jun-17, Volume: 363, Issue:3 Topics: Adult; Aged; Analysis of Variance; Antiparkinson Agents; Area Under Curve; Benserazide; Biological A	2004
Genetic polymorphism of catechol-O-methyltransferase and levodopa pharmacokinetic-pharmacodynamic pattern in patients with Parkinson's disease. Movement disorders : official journal of the Movement Disorder Society, 2005, Volume: 20, Issue:6 Topics: Aged; Analysis of Variance; Antiparkinson Agents; Area Under Curve; Benserazide; Catechol O-Methyltr	2005
Acute levodopa administration reduces cortisol release in patients with Parkinson's disease. Journal of neural transmission (Vienna, Austria : 1996), 2007, Volume: 114, Issue:3 Topics: Aged; Antiparkinson Agents; Benserazide; Down-Regulation; Enzyme Inhibitors; Humans; Hydrocortisone;	2007
[Clinical observation on abdominal acupuncture plus Madopa for treatment of Parkinson's disease]. Zhongguo zhen jiu = Chinese acupuncture & moxibustion, 2007, Volume: 27, Issue:8 Topics: Abdomen; Acupuncture Therapy; Adult; Aged; Benserazide; Drug Combinations; Female; Humans; Levodopa;	2007
[Effect of TCM treatment according to syndrome differentiation in enhancing curative effect and reducing side-effect of madopa]. Zhongguo Zhong xi yi jie he za zhi Zhongguo Zhongxiyi jiehe zazhi = Chinese journal of integrated traditional and Western medicine, 2007, Volume: 27, Issue:9 Topics: Aged; Aged, 80 and over; Benserazide; Diagnosis, Differential; Dopamine Agents; Drug Combinations; D	2007
Impact of endurance exercise on levodopa-associated cortisol release and force increase in patients with Parkinson's disease. Journal of neural transmission (Vienna, Austria : 1996), 2008, Volume: 115, Issue:6 Topics: Adult; Aged; Antiemetics; Antiparkinson Agents; Benserazide; Domperidone; Drug Administration Schedu	2008
[Combined treatment of the early stages of Parkinson's syndrome with bromocriptine and levodopa. The results of a multicenter study]. Deutsche medizinische Wochenschrift (1946), 1984, Aug-24, Volume: 109, Issue:34 Topics: Aged; Benserazide; Bromocriptine; Chronic Disease; Clinical Trials as Topic; Drug Therapy, Combinati	1984
[A new levodopa benserazide preparation for Parkinson's disease with motor fluctuations refractory to standard L-dopa]. Medicina, 1991, Volume: 51, Issue:6 Topics: Adult; Aged; Benserazide; Drug Combinations; Female; Humans; Levodopa; Male; Middle Aged; Movement D	1991
The therapeutic potential of moclobemide, a reversible selective monoamine oxidase A inhibitor in Parkinson's disease. Journal of clinical psychopharmacology, 1995, Volume: 15, Issue:4 Suppl 2 Topics: Adult; Affect; Aged; Aged, 80 and over; Antiparkinson Agents; Benserazide; Benzamides; Cognition; Dr	1995
[Slow-release L-dopa vs. standard L-dopa in Parkinson patients in various stages of the disease. Studies of pharmacokinetics and motor effectiveness]. Der Nervenarzt, 1994, Volume: 65, Issue:4 Topics: Adult; Aged; Benserazide; Delayed-Action Preparations; Double-Blind Method; Drug Combinations; Femal	1994
Visual control of arm movement in Parkinson's disease. Movement disorders : official journal of the Movement Disorder Society, 1994, Volume: 9, Issue:1 Topics: Adult; Aged; Attention; Benserazide; Bromocriptine; Drug Therapy, Combination; Female; Humans; Levod	1994
Defining small differences in efficacy between anti-parkinsonian agents using gait analysis: a comparison of two controlled release formulations of levodopa/decarboxylase inhibitor. British journal of clinical pharmacology, 1993, Volume: 35, Issue:4 Topics: Aged; Analysis of Variance; Antiparkinson Agents; Benserazide; Carbidopa; Carboxy-Lyases; Delayed-Ac	1993
Comparison of therapeutic effects and mortality data of levodopa and levodopa combined with selegiline in patients with early, mild Parkinson's disease. Parkinson's Disease Research Group of the United Kingdom. BMJ (Clinical research ed.), 1995, Dec-16, Volume: 311, Issue:7020 Topics: Antiparkinson Agents; Benserazide; Bromocriptine; Cause of Death; Disability Evaluation; Drug Admini	1995
'Atypical' tremor. European neurology, 1995, Volume: 35, Issue:6 Topics: Benserazide; Child; Child, Preschool; Cross-Over Studies; Double-Blind Method; Drug Combinations; El	1995
A study on the effect and tolerance of lisuride on Parkinson's disease. Advances in neurology, 1996, Volume: 69 Topics: Age of Onset; Aged; Antiparkinson Agents; Benserazide; Disease Progression; Drug Therapy, Combinatio	1996
Acute administration of levodopa-benserazide and tolcapone, a COMT inhibitor, Parkinson's disease. Clinical neuropharmacology, 1995, Volume: 18, Issue:3 Topics: Aged; Antiparkinson Agents; Benserazide; Benzophenones; Catechol O-Methyltransferase Inhibitors; Dos	1995
Sustained-release Madopar HBS compared with standard Madopar in the long-term treatment of de novo parkinsonian patients. Acta neurologica Scandinavica, 1996, Volume: 93, Issue:1 Topics: Aged; Antiparkinson Agents; Benserazide; Delayed-Action Preparations; Denmark; Dose-Response Relatio	1996
An add-on study of selegiline to Madopar in the treatment of parkinsonian patients with dose-related fluctuations: comparison between Jumexal and Parkryl. Zhonghua yi xue za zhi = Chinese medical journal; Free China ed, 1996, Volume: 58, Issue:4 Topics: Aged; Antiparkinson Agents; Benserazide; Cross-Over Studies; Dose-Response Relationship, Drug; Drug	1996
Clinical efficacy and tolerability of a new levodopa/benserazide dual-release formulation in parkinsonian patients. L-Dopa Dual-Release Study Group. Clinical neuropharmacology, 1997, Volume: 20, Issue:2 Topics: Aged; Aged, 80 and over; Antiparkinson Agents; Aromatic Amino Acid Decarboxylase Inhibitors; Bensera	1997
Comparison of subcutaneous apomorphine versus dispersible madopar latency and effect duration in Parkinson's disease patients: a double-blind single-dose study. Clinical neuropharmacology, 1997, Volume: 20, Issue:2 Topics: Administration, Oral; Antiparkinson Agents; Apomorphine; Aromatic Amino Acid Decarboxylase Inhibitor	1997
Simultaneous MAO-B and COMT inhibition in L-Dopa-treated patients with Parkinson's disease. Movement disorders : official journal of the Movement Disorder Society, 1997, Volume: 12, Issue:4 Topics: Aged; Analysis of Variance; Antiparkinson Agents; Benserazide; Catechol O-Methyltransferase Inhibito	1997
Postural tremor of Parkinson's disease. Clinical neuropharmacology, 1994, Volume: 17, Issue:3 Topics: Adult; Aged; Antiparkinson Agents; Benserazide; Electromyography; Female; Humans; Levodopa; Male; Mi	1994
Catechol-O-methyltransferase inhibition with tolcapone reduces the "wearing off" phenomenon and levodopa requirements in fluctuating parkinsonian patients. Neurology, 1998, Volume: 50, Issue:5 Suppl 5 Topics: Aged; Antiparkinson Agents; Benserazide; Benzophenones; Catechol O-Methyltransferase Inhibitors; Dia	1998
The effect of tolcapone on the pharmacokinetics of benserazide. European journal of neurology, 1999, Volume: 6, Issue:2 Topics: Aged; Antiparkinson Agents; Benserazide; Benzophenones; Dose-Response Relationship, Drug; Drug Admin	1999
COMT inhibition by tolcapone further improves levodopa pharmacokinetics when combined with a dual-release formulation of levodopa/benserazide. A novel principle in the treatment of Parkinson's disease. European neurology, 1999, Volume: 41, Issue:4 Topics: Adolescent; Adult; Antiparkinson Agents; Benserazide; Benzophenones; Catechol O-Methyltransferase; C	1999
Population pharmacokinetics of tolcapone in parkinsonian patients in dose finding studies. British journal of clinical pharmacology, 2000, Volume: 49, Issue:1 Topics: Adult; Aged; Aged, 80 and over; Analysis of Variance; Antiparkinson Agents; Area Under Curve; Benser	2000
[Efficiency of new forms of madopar in Parkinson's disease]. Zhurnal nevrologii i psikhiatrii imeni S.S. Korsakova, 2000, Volume: 100, Issue:12 Topics: Antiparkinson Agents; Benserazide; Dose-Response Relationship, Drug; Drug Combinations; Female; Huma	2000
Dual-release formulation, a novel principle in L-dopa treatment of Parkinson's disease. Neurology, 2001, May-08, Volume: 56, Issue:9 Topics: Aged; Benserazide; Delayed-Action Preparations; Double-Blind Method; Drug Combinations; Humans; Levo	2001
Delay of simple reaction time after levodopa intake. Clinical neurophysiology : official journal of the International Federation of Clinical Neurophysiology, 2001, Volume: 112, Issue:11 Topics: Adult; Aged; Antiparkinson Agents; Behavior; Benserazide; Cognition; Dopamine Agents; Drug Combinati	2001
Levodopa alone and in combination with a peripheral decarboxylase inhibitor benserazide (Madopar) in the treatment of Parkinson's disease: A controlled clinical trial. Journal of neurology, 1975, Dec-02, Volume: 211, Issue:1 Topics: Adult; Aged; Aromatic Amino Acid Decarboxylase Inhibitors; Benserazide; Blood Pressure; Clinical Tri	1975
Implications of combined treatment with 'Madopar' and L-deprenil in Parkinson's disease. A long-term study. Lancet (London, England), 1977, Feb-26, Volume: 1, Issue:8009 Topics: Administration, Oral; Aged; Benserazide; Clinical Trials as Topic; Disability Evaluation; Drug Combi	1977
Comparison of levodopa with carbidopa or benserazide in parkinsonism. Lancet (London, England), 1976, Aug-21, Volume: 2, Issue:7982 Topics: Aged; Benserazide; Carbidopa; Consumer Behavior; Drug Administration Schedule; Drug Evaluation; Drug	1976
[Levodopa and decarboxylase inhibitors in Parkinson's disease]. Lakartidningen, 1977, Jan-05, Volume: 74, Issue:1-2 Topics: Adult; Aged; Benserazide; Clinical Trials as Topic; Drug Evaluation; Female; Humans; Hydrazines; Lev	1977
Long-term treatment of Parkinson's disease with L-Dopa and Dopa-decarboxylase inhibitor: therapeutic results and side effects. Acta neurologica Scandinavica, 1978, Volume: 57, Issue:2 Topics: Aromatic Amino Acid Decarboxylase Inhibitors; Benserazide; Carbidopa; Clinical Trials as Topic; Drug	1978
A double-blind comparison of levodopa, Madopa, and Sinemet in Parkinson disease. Annals of neurology, 1978, Volume: 3, Issue:3 Topics: Adult; Benserazide; Carbidopa; Clinical Trials as Topic; Double-Blind Method; Drug Combinations; Fem	1978
Levodopa/benserazide ('Madopar') combination therapy in elderly patients with parkinsonism. Current medical research and opinion, 1979, Volume: 6, Issue:1 Topics: Activities of Daily Living; Aged; Benserazide; Clinical Trials as Topic; Drug Combinations; Female;	1979
[The combined treatment of Parkinson's disease with L-dopa plus decarboxylase inhibitors (carbidopa, benserazide) (author's transl)]. Wiener klinische Wochenschrift, 1979, May-11, Volume: 91, Issue:10 Topics: Aged; Benserazide; Carbidopa; Drug Combinations; Drug Evaluation; Female; Humans; Hydrazines; Levodo	1979
Levodopa with benserazide or carbidopa in Parkinson disease. Neurology, 1979, Volume: 29, Issue:12 Topics: Benserazide; Biological Availability; Carbidopa; Dose-Response Relationship, Drug; Drug Therapy, Com	1979
Effect of CB 154 (2-bromo-alpha-ergocryptine) on paralysis agitans compared with Madopar in a double-blind, cross-over trial. Acta neurologica Scandinavica, 1976, Volume: 53, Issue:3 Topics: Aged; Azides; Benserazide; Bromocriptine; Clinical Trials as Topic; Dose-Response Relationship, Drug	1976
[Sinomet and Madopar, a comparative study on the treatment of Parkinson's disease]. Nederlands tijdschrift voor geneeskunde, 1976, Oct-02, Volume: 120, Issue:40 Topics: Benserazide; Carbidopa; Clinical Trials as Topic; Drug Combinations; Drug Evaluation; Humans; Levodo	1976
Madopar versus sinemet. A clinical study on their effectiveness. European neurology, 1975, Volume: 13, Issue:2 Topics: Adult; Aged; Benserazide; Carbidopa; Clinical Trials as Topic; Drug Evaluation; Female; Humans; Hydr	1975
Indications of piribedil in L-DOPA-treated parkinsonian patients: physiopathologic implications. Advances in neurology, 1975, Volume: 9 Topics: Adult; Aged; Benserazide; Clinical Trials as Topic; Drug Evaluation; Female; Humans; Levodopa; Male;	1975
Parkinson's disease treated with Sinemet or Madopar. A controlled multicenter trial. Acta neurologica Scandinavica, 1976, Volume: 53, Issue:5 Topics: Aged; Benserazide; Carbidopa; Drug Combinations; Drug Evaluation; Female; Humans; Hydrazines; Levodo	1976
Primary combination therapy of early Parkinson's disease. A long-term comparison between the combined regimen bromocriptine/levodopa and levodopa monotherapy--first interim report. European neurology, 1992, Volume: 32 Suppl 1 Topics: Benserazide; Bromocriptine; Dose-Response Relationship, Drug; Drug Therapy, Combination; Humans; Lev	1992
Comparative efficacy of two oral sustained-release preparations of L-dopa in fluctuating Parkinson's disease. Preliminary findings in 20 patients. Journal of neural transmission. Parkinson's disease and dementia section, 1992, Volume: 4, Issue:2 Topics: Benserazide; Carbidopa; Delayed-Action Preparations; Drug Combinations; Follow-Up Studies; Humans; L	1992
A single-dose study of the pharmacodynamic effects of chlormethiazole, temazepam and placebo in elderly parkinsonian patients. Age and ageing, 1991, Volume: 20, Issue:6 Topics: Aged; Benserazide; Carbidopa; Chlormethiazole; Double-Blind Method; Drug Therapy, Combination; Femal	1991
A comparison of standard Madopar and controlled release Madopar in Parkinson's disease. Australian and New Zealand journal of medicine, 1991, Volume: 21, Issue:1 Topics: Adult; Aged; Benserazide; Carboxy-Lyases; Delayed-Action Preparations; Dose-Response Relationship, D	1991
Controlled-release levodopa/benserazide (Madopar HBS): clinical observations and levodopa and dopamine plasma concentrations in fluctuating parkinsonian patients. Journal of neurology, 1990, Volume: 237, Issue:1 Topics: Aged; Benserazide; Carboxy-Lyases; Clinical Trials as Topic; Delayed-Action Preparations; Dopamine;	1990
A comparison of the effects of controlled-release levodopa (Madopar CR) with conventional levodopa in late Parkinson's disease. Journal of neurology, neurosurgery, and psychiatry, 1990, Volume: 53, Issue:3 Topics: Adult; Aged; Aged, 80 and over; Benserazide; Carboxy-Lyases; Delayed-Action Preparations; Dose-Respo	1990
Levodopa treatment of Parkinson's syndrome: past and future. Advances in neurology, 1990, Volume: 53 Topics: Benserazide; Brain; Carboxy-Lyases; Drug Therapy, Combination; Forecasting; Humans; Levodopa; Parkin	1990
Madopar HBS (hydrodynamically balanced system) in the treatment of Parkinson's disease. Advances in neurology, 1990, Volume: 53 Topics: Aged; Antiparkinson Agents; Benserazide; Circadian Rhythm; Delayed-Action Preparations; Drug Adminis	1990
Madopar HBS in nocturnal symptoms of Parkinson's disease. Advances in neurology, 1990, Volume: 53 Topics: Adult; Aged; Benserazide; Carboxy-Lyases; Circadian Rhythm; Delayed-Action Preparations; Dose-Respon	1990
Open study of sustained-release formulation of levodopa and benserazide in parkinsonian patients. Neurologija, 1990, Volume: 39, Issue:2 Topics: Adult; Benserazide; Delayed-Action Preparations; Drug Combinations; Drug Therapy, Combination; Femal	1990
Effectiveness of Madopar HBS plus Madopar standard in patients with fluctuating Parkinson's disease: two years of follow-up. European neurology, 1990, Volume: 30, Issue:6 Topics: Adult; Aged; Benserazide; Delayed-Action Preparations; Drug Combinations; Drug Therapy, Combination;	1990
Tetrahydrobiopterin and Parkinson's disease. Acta neurologica Scandinavica, 1989, Volume: 79, Issue:6 Topics: Adult; Antiparkinson Agents; Benserazide; Biopterins; Clinical Trials as Topic; Drug Combinations; H	1989
A comparison of Madopar CR and standard Madopar in the treatment of nocturnal and early-morning disability in Parkinson's disease. The U.K. Madopar CR Study Group. Clinical neuropharmacology, 1989, Volume: 12, Issue:6 Topics: Activities of Daily Living; Aged; Benserazide; Circadian Rhythm; Delayed-Action Preparations; Double	1989
A combined regimen of subcutaneous lisuride and oral Madopar HBS in Parkinson's disease. Journal of neural transmission. Supplementum, 1988, Volume: 27 Topics: Administration, Oral; Benserazide; Clinical Trials as Topic; Drug Administration Schedule; Drug Comb	1988
A controlled release form of madopar in parkinsonian patients with advanced disease and marked fluctuations in motor performance. Acta neurologica Scandinavica, 1988, Volume: 77, Issue:5 Topics: Benserazide; Clinical Trials as Topic; Delayed-Action Preparations; Drug Administration Schedule; Dr	1988
Madopar HBS in fluctuating parkinsonian patients: two-year treatment. Movement disorders : official journal of the Movement Disorder Society, 1988, Volume: 3, Issue:1 Topics: Adult; Aged; Benserazide; Carboxy-Lyases; Clinical Trials as Topic; Delayed-Action Preparations; Dru	1988
The effect of R-(-)-deprenyl in de novo Parkinson patients on combination therapy with levodopa and decarboxylase inhibitor. Journal of neural transmission. Supplementum, 1987, Volume: 25 Topics: Benserazide; Clinical Trials as Topic; Disability Evaluation; Drug Therapy, Combination; Female; Hum	1987
Adjuvant treatment of Parksinson's disease with budipine: a double-blind trial versus placebo. Journal of neurology, 1987, Volume: 234, Issue:5 Topics: Aged; Aged, 80 and over; Antiparkinson Agents; Benserazide; Clinical Trials as Topic; Double-Blind M	1987
Clinical trial of Madopar HBS in parkinsonian patients with fluctuating drug response after long-term levodopa therapy. European neurology, 1987, Volume: 27 Suppl 1 Topics: Aged; Benserazide; Clinical Trials as Topic; Delayed-Action Preparations; Drug Combinations; Female;	1987
Open study of Madopar HBS, a new formulation of levodopa with benserazide, in 13 patients with Parkinson's disease and 'on-off' fluctuations. European neurology, 1987, Volume: 27 Suppl 1 Topics: Adult; Aged; Benserazide; Clinical Trials as Topic; Delayed-Action Preparations; Dose-Response Relat	1987
Single-dose studies of a slow-release preparation of levodopa and benserazide (Madopar HBS) in Parkinson's disease. European neurology, 1987, Volume: 27 Suppl 1 Topics: Administration, Oral; Adult; Aged; Benserazide; Biological Availability; Clinical Trials as Topic; D	1987
Open clinical study of Madopar HBS. European neurology, 1987, Volume: 27 Suppl 1 Topics: Adult; Aged; Benserazide; Clinical Trials as Topic; Delayed-Action Preparations; Dose-Response Relat	1987
Treatment of parkinsonian conditions with a controlled-release form of levodopa--preliminary study. European neurology, 1987, Volume: 27 Suppl 1 Topics: Adult; Aged; Benserazide; Clinical Trials as Topic; Delayed-Action Preparations; Dose-Response Relat	1987
Preliminary experience with Madopar HBS: clinical observations and plasma levodopa concentrations. European neurology, 1987, Volume: 27 Suppl 1 Topics: Adult; Aged; Benserazide; Clinical Trials as Topic; Delayed-Action Preparations; Drug Combinations;	1987
Clinical and pharmacokinetic observations with Madopar HBS in hospitalized patients with Parkinson's disease and motor fluctuations. European neurology, 1987, Volume: 27 Suppl 1 Topics: Benserazide; Clinical Trials as Topic; Delayed-Action Preparations; Dose-Response Relationship, Drug	1987
Open multicenter trial with Madopar HBS in parkinsonian patients. Preliminary assessment after short-term treatment. European neurology, 1987, Volume: 27 Suppl 1 Topics: Aged; Benserazide; Clinical Trials as Topic; Delayed-Action Preparations; Dose-Response Relationship	1987
Levodopa and monoamine oxidase inhibitor combination therapy. A controlled clinical trial. Journal of neural transmission. Supplementum, 1987, Volume: 25 Topics: Aged; Benserazide; Clinical Trials as Topic; Double-Blind Method; Drug Therapy, Combination; Female;	1987
[Controlled release levodopa-benserazide and changes in efficacy during treatment of Parkinson's disease]. Revue neurologique, 1987, Volume: 143, Issue:11 Topics: Adult; Aged; Benserazide; Carboxy-Lyases; Clinical Trials as Topic; Delayed-Action Preparations; Dru	1987
Mesulergine in early Parkinson's disease: a double blind controlled trial. Journal of neurology, neurosurgery, and psychiatry, 1986, Volume: 49, Issue:4 Topics: Aged; Antiparkinson Agents; Benserazide; Clinical Trials as Topic; Double-Blind Method; Drug Combina	1986
Single-dose study of slow release preparation of levodopa and benserazide (Madopar HBS) in Parkinson's disease. Advances in neurology, 1987, Volume: 45 Topics: Administration, Oral; Aged; Benserazide; Clinical Trials as Topic; Delayed-Action Preparations; Disa	1987
Patient benefits of l-dopa and a decarboxylase inhibitor in the treatment of Parkinson's disease in elderly patients. Pharmatherapeutica, 1985, Volume: 4, Issue:2 Topics: Activities of Daily Living; Aged; Aromatic Amino Acid Decarboxylase Inhibitors; Benserazide; Carbido	1985
[2-year experiences with a combination treatment of Parkinsonism with L-dopa and a decarboxylase inhibitor (Benserazid, Ro 4-4602)]. Wiener medizinische Wochenschrift (1946), 1974, Jun-01, Volume: 124, Issue:22 Topics: Benserazide; Carboxy-Lyases; Clinical Trials as Topic; Dermatitis, Seborrheic; Dihydroxyphenylalanin	1974
[Experiences in the treatment of Parkinson's disease with a combination drug: L-dopa plus decarboxylase inhibitor (Ro 8-0576)]. Wiener medizinische Wochenschrift (1946), 1973, Jun-30, Volume: 123, Issue:26 Topics: Benserazide; Carboxy-Lyases; Clinical Trials as Topic; Dihydroxyphenylalanine; Drug Combinations; Ev	1973
Report on 45-month treatment of parkinsonism with L-dopa, alone and in association with a decarboxilase inhibitor (Ro 4-4602). Acta neurologica latinoamericana, 1974, Volume: 20, Issue:1-4 Topics: Adult; Aged; Benserazide; Clinical Trials as Topic; Drug Therapy, Combination; Female; Humans; Hydra	1974

benserazide and Parkinson Disease