PURINE SUBSTRATES FOR HUMAN THIOPURINE METHYLTRANSFERASE

被引：60

作者：

DEININGER, M ^{[1
]}

SZUMLANSKI, CL ^{[1
]}

OTTERNESS, DM ^{[1
]}

VANLOON, J ^{[1
]}

FERBER, W ^{[1
]}

WEINSHILBOUM, RM ^{[1
]}

机构：

[1] MAYO CLIN & MAYO FDN,MAYO MED SCH,DEPT PHARMACOL,ROCHESTER,MN 55905

来源：

BIOCHEMICAL PHARMACOLOGY | 1994年 / 48卷 / 11期

关键词：

THIOPURINE METHYLTRANSFERASE; THIOPURINES; METHYLATION; PHARMACOGENETICS;

D O I：

10.1016/0006-2952(94)90515-0

中图分类号：

R9 [药学];

学科分类号：

1007 ;

摘要：

Thiopurine methyltransferase (TPMT) catalyzes the S-methylation of thiopurine drugs such as 6-mercaptopurine (6-MP) and 6-thioguanine (6-TG). A genetic polymorphism regulating TPMT activity in human tissue is an important factor responsible for individual differences in the toxicity and therapeutic efficacy of these drugs. Because of the clinical importance of this polymorphism, we studied 18 purine derivatives, including ribonucleosides and ribonucleotides, as potential substrates for purified human kidney TPMT. Sixteen of the compounds studied were substrates for the enzyme, with K-m values that varied from 29.1 to 1270 mu M and with V-max, values that varied from 75 to 2340 U/mg protein. The thiopurines tested had K-m values that were uniformly lower than were those of the corresponding ribonucleosides or ribonucleotides. 6-Selenopurine derivatives had the lowest K-m values of the compounds studied. Finally, oxidized purines with an OH in the and-position were methylated by the enzyme, but 2-OH compounds were potent inhibitors of TPMT.

引用

页码：2135 / 2138

页数：4

共 25 条

[1] THIOPURINE METHYLTRANSFERASE - STRUCTURE-ACTIVITY-RELATIONSHIPS FOR BENZOIC-ACID INHIBITORS AND THIOPHENOL SUBSTRATES [J].

AMES, MM ;

SELASSIE, CD ;

WOODSON, LC ;

VANLOON, JA ;

HANSCH, C ;

WEINSHILBOUM, RM .

JOURNAL OF MEDICINAL CHEMISTRY, 1986, 29 (03) :354-358

[2]

BRADFORD MM, 1976, ANAL BIOCHEM, V72, P248, DOI 10.1016/0003-2697(76)90527-3

[3] COMPUTER PROGRAMMES FOR PROCESSING ENZYME KINETIC DATA [J].

CLELAND, WW .

NATURE, 1963, 198 (487) :463-+

[4]

ELION GB, 1967, FED PROC, V26, P898

[5] FORMATION OF DIMETHYL SELENIDE AND TRIMETHYLSELENONIUM FROM SELENOBETAINE IN THE RAT [J].

FOSTER, SJ ;

KRAUS, RJ ;

GANTHER, HE .

ARCHIVES OF BIOCHEMISTRY AND BIOPHYSICS, 1986, 247 (01) :12-19

[6] HUMAN LIVER XANTHINE-OXIDASE - NATURE AND EXTENT OF INDIVIDUAL VARIATION [J].

GUERCIOLINI, R ;

SZUMLANSKI, C ;

WEINSHILBOUM, RM .

CLINICAL PHARMACOLOGY & THERAPEUTICS, 1991, 50 (06) :663-672

[7]

HONCHEL R, 1993, MOL PHARMACOL, V43, P878

[8] COMPARISON OF SPECIFICITIES OF XANTHINE-OXIDASE AND ALDEHYDE OXIDASE [J].

KRENITSKY, TA ;

ELION, GB ;

HITCHINGS, GH ;

NEIL, SM .

ARCHIVES OF BIOCHEMISTRY AND BIOPHYSICS, 1972, 150 (02) :585-+

[9] THIOPURINE PHARMACOGENETICS IN LEUKEMIA - CORRELATION OF ERYTHROCYTE THIOPURINE METHYLTRANSFERASE ACTIVITY AND 6-THIOGUANINE NUCLEOTIDE CONCENTRATIONS [J].

LENNARD, L ;

VANLOON, JA ;

LILLEYMAN, JS ;

WEINSHILBOUM, RM .

CLINICAL PHARMACOLOGY & THERAPEUTICS, 1987, 41 (01) :18-25

[10] IS 6-THIOGUANINE MORE APPROPRIATE THAN 6-MERCAPTOPURINE FOR CHILDREN WITH ACUTE LYMPHOBLASTIC-LEUKEMIA [J].

LENNARD, L ;

DAVIES, HA ;

LILLEYMAN, JS .

BRITISH JOURNAL OF CANCER, 1993, 68 (01) :186-190

← 1 2 3 →