TOXICOLOGY OF QUINONE-THIOETHERS

被引：124

作者：

MONKS, TJ

LAU, SS

机构：

[1] Division of Pharmacology and Toxicology, College of Pharmacy, The University of Texas at Austin, Austin

来源：

CRITICAL REVIEWS IN TOXICOLOGY | 1992年 / 22卷 / 5-6期

关键词：

QUINONES; GLUTATHIONE; QUINONE-THIOETHERS; GLUTATHIONE CONJUGATES; NEPHROTOXICITY; NEPHROCARCINOGENICITY; NEUROTOXICITY;

D O I：

10.3109/10408449209146309

中图分类号：

R99 [毒物学（毒理学）];

学科分类号：

100405 ;

摘要：

Cytotoxicity associated with exposure to quinones has generally been attributed to either redox cycling, and the subsequent development of ''oxidative stress.'' and/or to their interaction with cellular nucleophiles, such as protein and non-protein sulfhydryls. Glutathione (GSH) is the major non-protein sulfhydryl present in cells, and conjugation of potentially toxic electrophiles with GSH is usually associated with detoxication and excretion. However, this review discusses the biological (re)activity of quinone-thioethers. For example, quinone-thioethers are (1) capable of redox cycling (2) substrates for, and inhibitors of, a variety of enzymes (3) methemoglobinemic (4) potent nephrotoxicants (5) DNA reactive and (6) may contribute to quinone-mediated carcinogenicity and neurotoxicity. The ubiquitous nature of quinones, and the high intracellular concentrations of GSH, ensures that cells and tissues will be exposed to quinone-thioethers. The toxicological importance of quinone-thioethers in quinone-mediated toxicities therefore deserves further attention.

引用

页码：243 / 270

页数：28

共 188 条

[1] DIETARY CARCINOGENS AND ANTICARCINOGENS - OXYGEN RADICALS AND DEGENERATIVE DISEASES
AMES, BN
[J]. SCIENCE, 1983, 221 (4617) : 1256 - 1264
[2] BIOSYNTHESIS AND BIOTRANSFORMATION OF GLUTATHIONE S-CONJUGATES TO TOXIC METABOLITES
ANDERS, MW
LASH, L
DEKANT, W
ELFARRA, AA
DOHN, DR
[J]. CRC CRITICAL REVIEWS IN TOXICOLOGY, 1988, 18 (04): : 311 - 341
[3] HYDROPEROXIDE-DEPENDENT ACTIVATION OF PARA-PHENETIDINE CATALYZED BY PROSTAGLANDIN SYNTHASE AND OTHER PEROXIDASES
ANDERSSON, B
LARSSON, R
RAHIMTULA, A
MOLDEUS, P
[J]. BIOCHEMICAL PHARMACOLOGY, 1983, 32 (06) : 1045 - 1050
[4] PROSTAGLANDIN SYNTHASE AND HORSERADISH-PEROXIDASE CATALYZED DNA-BINDING OF PARA-PHENETIDINE
ANDERSSON, B
LARSSON, R
RAHIMTULA, A
MOLDEUS, P
[J]. CARCINOGENESIS, 1984, 5 (02) : 161 - 165
[5] ELECTROPHORETIC MOBILITY OF GAMMA-GLUTAMYLTRANSFERASE IN RAT-LIVER SUBCELLULAR-FRACTIONS - EVIDENCE FOR STRUCTURE DIFFERENCE FROM THE KIDNEY ENZYME
ANTOINE, B
VISVIKIS, A
THIOUDELLET, C
RAHIMIPOUR, A
STRAZIELLE, N
WELLMAN, M
SIEST, G
[J]. BIOCHEMICAL JOURNAL, 1989, 262 (02) : 535 - 539
[6] AUGUSTEYN RC, 1981, MECHANISMS CATARACT, P71
[7] BALL P, 1983, CATECHOL ESTROGENS, P91
[8] BARANCZYKKUZMA A, 1986, J NEUROCHEM, V46, P1956
[9] CHEMICAL SYMPATHECTOMY INDUCED BY 5,6-DIHYDROXYTRYPTAMINE
BAUMGARTEN, HG
SCHLOSSBERGER, HG
GOTHERT, M
HOLSTEIN, AF
[J]. ZEITSCHRIFT FUR ZELLFORSCHUNG UND MIKROSKOPISCHE ANATOMIE, 1972, 128 (01): : 115 - +
[10] EFFECTS OF 5,6-DIHYDROXYTRYPTAMINE ON MONOAMINERGIC NEURONS IN CENTRAL NERVOUS-SYSTEM OF RAT
BAUMGARTEN, HG
IVERSEN, LL
WILSON, G
VOGT, M
HOLMAN, RB
EVETTS, KD
[J]. JOURNAL OF NEUROCHEMISTRY, 1972, 19 (06) : 1587 - +

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