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DEBRISOQUINE HYDROXYLATION IN PARKINSONS-DISEASE

被引:30
作者
STEIGER, MJ
LLEDO, P
QUINN, NP
MARSDEN, CD
TURNER, P
JENNER, PG
机构
[1] NAT HOSP NEUROL & NEUROSURG,INST NEUROL,DEPT CLIN NEUROL,LONDON,ENGLAND
[2] UNIV LONDON KINGS COLL,DIV BIOMED SCI,PHARMACOL GRP,PARKINSONS DIS SOC EXPTL RES LAB,LONDON WC2R 2LS,ENGLAND
[3] ST BARTHOLOMEWS HOSP,DEPT CLIN PHARMACOL,LONDON EC1A 7BE,ENGLAND
来源
ACTA NEUROLOGICA SCANDINAVICA | 1992年 / 86卷 / 02期
关键词
PARKINSONS DISEASE; DEBRISOQUINE METABOLISM; ENVIRONMENTAL TOXINS;
D O I
10.1111/j.1600-0404.1992.tb05059.x
中图分类号
R74 [神经病学与精神病学];
学科分类号
摘要
Debrisoquine (DBQ) metabolism was studied in 80 Parkinson's disease (PD) patients, 26 of whom had young onset Parkinson's disease (YOPD), and in 143 controls. There was no significant difference between the proportion of poor metabolisers of DBQ among YOPD patients compared either to other parkinsonians, or to controls. Nor was there a significant correlation between the age of disease onset and DBQ metabolic ratio (MR). The results do not support the suggestion that impairment of DBQ metabolism (and hence cytochrome P450) is a primary defect in YOPD. However, in comparison with controls, MR values were modestly but significantly higher in PD patients, even in those not treated with drugs known to affect DBQ metabolism.
引用
收藏
页码:159 / 164
页数:6
相关论文
共 30 条
[1]  
BARBEAU A, 1985, LANCET, V2, P1213
[2]   OXIDATIVE POLYMORPHISM OF DEBRISOQUINE IN PARKINSONS-DISEASE [J].
BENITEZ, J ;
LADERO, JM ;
JIMENEZJIMENEZ, FJ ;
MARTINEZ, C ;
PUERTO, AM ;
VALDIVIELSO, MJ ;
LLERENA, A ;
COBALEDA, J ;
MUNOZ, JJ .
JOURNAL OF NEUROLOGY NEUROSURGERY AND PSYCHIATRY, 1990, 53 (04) :289-292
[3]   ETIOLOGY OF PARKINSONS-DISEASE [J].
CALNE, DB ;
LANGSTON, JW .
LANCET, 1983, 2 (8365) :1457-1459
[4]  
COMELLA CL, 1987, NEUROLOGY S, V1, P261
[5]   CHRONIC PARKINSONISM SECONDARY TO INTRAVENOUS-INJECTION OF MEPERIDINE ANALOGS [J].
DAVIS, GC ;
WILLIAMS, AC ;
MARKEY, SP ;
EBERT, MH ;
CAINE, ED ;
REICHERT, CM ;
KOPIN, IJ .
PSYCHIATRY RESEARCH, 1979, 1 (03) :249-254
[6]  
EICHELBAUM M, 1986, BR J CLIN PHARM, V23, P455
[7]   A FAMILY AND POPULATION STUDY OF THE GENETIC-POLYMORPHISM OF DEBRISOQUINE OXIDATION IN A WHITE BRITISH-POPULATION [J].
EVANS, DAP ;
MAHGOUB, A ;
SLOAN, TP ;
IDLE, JR ;
SMITH, RL .
JOURNAL OF MEDICAL GENETICS, 1980, 17 (02) :102-105
[8]   MPTP, THE NEUROTOXIN INDUCING PARKINSONS-DISEASE, IS A POTENT COMPETITIVE INHIBITOR OF HUMAN AND RAT CYTOCHROME-P450 ISOZYMES (P450BUFI, P450DB1) CATALYZING DEBRISOQUINE 4-HYDROXYLATION [J].
FONNEPFISTER, R ;
BARGETZI, MJ ;
MEYER, UA .
BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1987, 148 (03) :1144-1150
[9]   XENOBIOTIC AND ENDOBIOTIC INHIBITORS OF CYTOCHROME-P-450DBL FUNCTION, THE TARGET OF THE DEBRISOQUINE SPARTEINE TYPE POLYMORPHISM [J].
FONNEPFISTER, R ;
MEYER, UA .
BIOCHEMICAL PHARMACOLOGY, 1988, 37 (20) :3829-3835
[10]   POOR HYDROXYLATOR PHENOTYPES OF DEBRISOQUINE AND S-MEPHENYTOIN ARE NOT OVER-REPRESENTED IN A GROUP OF PATIENTS WITH PARKINSONS-DISEASE [J].
GUDJONSSON, O ;
SANZ, E ;
ALVAN, G ;
AOUILONIUS, SM ;
REVIRIEGO, J .
BRITISH JOURNAL OF CLINICAL PHARMACOLOGY, 1990, 30 (02) :301-302
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