PHARMACOGENETIC PHENOTYPING AND GENOTYPING - PRESENT STATUS AND FUTURE POTENTIAL

被引：176

作者：

GONZALEZ, FJ

IDLE, JR

机构：

[1] UNIV NEWCASTLE UPON TYNE,SCH MED,DEPT PHARMACOL SCI,PHARMACOGENET UNIT,NEWCASTLE TYNE,TYNE & WEAR,ENGLAND

[2] GENOTYPE LTD,NEWCASTLE TYNE,TYNE & WEAR,ENGLAND

来源：

CLINICAL PHARMACOKINETICS | 1994年 / 26卷 / 01期

关键词：

D O I：

10.2165/00003088-199426010-00005

中图分类号：

R9 [药学];

学科分类号：

1007 ;

摘要：

Enzymes that metabolise foreign compounds exhibit a large degree of interindividual variability in their levels of expression. In a number of instances this variability can be accounted for by null or variant alleles resulting from mutations in genes encoding these enzymes. Human variability in drug metabolism can be determined by biochemical and pharmacological assays. In cases where a genetic change has been characterised, polymerase chain reaction techniques have been developed to diagnose metabolism deficiencies. Genetic differences in certain foreign compound metabolising enzymes such as glutathione S-transferase M1, N-acetyltranferase 2 and CYP2D6 have been shown to be associated with risk for developing environmentally and occupationally based diseases such as cancer. Drug therapy can also be compromised by the existence of genetic deficiencies in a number of enzymes, including CYP2D6. It is anticipated that determination of an individual's drug metabolism capabilities by use of phenotyping and genotyping tests will allow for more rational and safe drug administration protocols.

引用

页码：59 / 70

页数：12

共 69 条

[1] PHARMACOGENETICS OF ALCOHOL METABOLISM AND ALCOHOLISM
AGARWAL, DP
GOEDDE, HW
[J]. PHARMACOGENETICS, 1992, 2 (02): : 48 - 62
[2] SLOW OMEPRAZOLE METABOLIZERS ARE ALSO POOR S-MEPHENYTOIN HYDROXYLATORS
ANDERSSON, T
REGARDH, CG
DAHLPUUSTINEN, ML
BERTILSSON, L
[J]. THERAPEUTIC DRUG MONITORING, 1990, 12 (04) : 415 - 416
[3] AOYAMA T, 1989, J BIOL CHEM, V264, P10388
[4] ATKINS S, 1993, AM J HUM GENET, V52, P598
[5] GENETIC RISK AND CARCINOGEN EXPOSURE - A COMMON INHERITED DEFECT OF THE CARCINOGEN-METABOLISM GENE GLUTATHIONE-S-TRANSFERASE M1 (GSTM1) THAT INCREASES SUSCEPTIBILITY TO BLADDER-CANCER
BELL, DA
TAYLOR, JA
PAULSON, DF
ROBERTSON, CN
MOHLER, JL
LUCIER, GW
[J]. JOURNAL OF THE NATIONAL CANCER INSTITUTE, 1993, 85 (14) : 1159 - 1164
[6] MOLECULAR MECHANISM OF SLOW ACETYLATION OF DRUGS AND CARCINOGENS IN HUMANS
BLUM, M
DEMIERRE, A
GRANT, DM
HEIM, M
MEYER, UA
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1991, 88 (12) : 5237 - 5241
[7] INDIVIDUAL VARIATION IN THE ACTIVATION AND INACTIVATION OF METABOLIC PATHWAYS OF CYCLOPHOSPHAMIDE
BODDY, AV
FURTUN, Y
SARDAS, S
SARDAS, O
IDLE, JR
[J]. JOURNAL OF THE NATIONAL CANCER INSTITUTE, 1992, 84 (22) : 1744 - 1748
[8] DEBRISOQUINE SPARTEINE HYDROXYLATION GENOTYPE AND PHENOTYPE - ANALYSIS OF COMMON MUTATIONS AND ALLELES OF CYP2D6 IN A EUROPEAN POPULATION
BROLY, F
GAEDIGK, A
HEIM, M
EICHELBAUM, M
MORIKE, K
MEYER, UA
[J]. DNA AND CELL BIOLOGY, 1991, 10 (08) : 545 - 558
[9] CLINICAL IMPLICATIONS OF VARIABLE ANTIARRHYTHMIC DRUG-METABOLISM
BUCHERT, E
WOOSLEY, RL
[J]. PHARMACOGENETICS, 1992, 2 (01): : 2 - 11
[10] DETERMINATION OF CYP1A2 AND NAT2 PHENOTYPES IN HUMAN-POPULATIONS BY ANALYSIS OF CAFFEINE URINARY METABOLITES
BUTLER, MA
LANG, NP
YOUNG, JF
CAPORASO, NE
VINEIS, P
HAYES, RB
TEITEL, CH
MASSENGILL, JP
LAWSEN, MF
KADLUBAR, FF
[J]. PHARMACOGENETICS, 1992, 2 (03): : 116 - 127

← 1 2 3 4 5 6 7 →