Mitochondrial targets of drug toxicity

被引：327

作者：

Wallace, KB ^{[1
]}

Starkov, AA ^{[1
]}

机构：

[1] Univ Minnesota, Sch Med, Dept Biochem & Mol Biol, Duluth, MN 55812 USA

来源：

ANNUAL REVIEW OF PHARMACOLOGY AND TOXICOLOGY | 2000年 / 40卷

关键词：

oxidative phosphorylation; uncouplers; bioenergetics; permeability transition; redox cycling;

D O I：

10.1146/annurev.pharmtox.40.1.353

中图分类号：

R9 [药学];

学科分类号：

1007 ;

摘要：

Mitochondria have long been recognized as the generators of energy for the cell. Like any other power source, however, mitochondria are highly vulnerable to inhibition or uncoupling of the energy harnessing process and run a high risk for catastrophic damage to the cell. The exquisite structural and functional characteristics of mitochondria provide a number of primary targets for xenobiotic-induced bioenergetic failure. They also provide opportunities for selective delivery of drugs to the mitochondrion. In light of the large number of natural, commercial, pharmaceutical, and environmental chemicals that manifest their toxicity by interfering with mitochondrial bioenergetics, it is important to understand the underlying mechanisms. The significance is further underscored by the recent identification of bioenergetic control points for cell replication and differentiation and the realization that mitochondria play a determinant role in cell signaling and apoptotic modes of cell death.

引用

页码：353 / 388

页数：36

共 187 条

[1] THE ATP-ADP-ANTIPORTER IS INVOLVED IN THE UNCOUPLING EFFECT OF FATTY-ACIDS ON MITOCHONDRIA [J].

ANDREYEV, AY ;

BONDAREVA, TO ;

DEDUKHOVA, VI ;

MOKHOVA, EN ;

SKULACHEV, VP ;

TSOFINA, LM ;

VOLKOV, NI ;

VYGODINA, TV .

EUROPEAN JOURNAL OF BIOCHEMISTRY, 1989, 182 (03) :585-592

[2] QUANTITATIVE STRUCTURE-ACTIVITY RELATIONSHIP OF CARBONYLCYANIDE PHENYLHYDRAZONES AS UNCOUPLERS OF MITOCHONDRIAL OXIDATIVE-PHOSPHORYLATION [J].

BALAZ, S ;

STURDIK, E ;

DURCOVA, E ;

ANTALIK, M ;

SULO, P .

BIOCHIMICA ET BIOPHYSICA ACTA, 1986, 851 (01) :93-98

[3] A CRITICAL-REVIEW OF THE LITERATURE ON HYDROGEN-SULFIDE TOXICITY [J].

BEAUCHAMP, RO ;

BUS, JS ;

POPP, JA ;

BOREIKO, CJ ;

ANDJELKOVICH, DA .

CRC CRITICAL REVIEWS IN TOXICOLOGY, 1984, 13 (01) :25-97

[4] UNCOUPLING OF RESPIRATORY-CHAIN PHOSPHORYLATION BY 4,5,6,7-TETRACHLORO-2-TRIFLUOROMETHYLBENZIMIDAZOLE [J].

BEECHEY, RB .

BIOCHEMICAL JOURNAL, 1966, 98 (01) :284-&

[5]

BERNARDI P, 1989, J BIOL CHEM, V264, P18902

[6] THE ROTENONE-INSENSITIVE REDUCTION OF QUINONES AND NITROCOMPOUNDS BY MITOCHONDRIAL NADH-UBIQUINONE REDUCTASE [J].

BIRONAITE, DA ;

CENAS, NK ;

KULYS, JJ .

BIOCHIMICA ET BIOPHYSICA ACTA, 1991, 1060 (02) :203-209

[7] INHIBITION OF MITOCHONDRIAL NADH OXIDASE, SUCCINOXIDASE, AND ATPASE BY NATURALLY-OCCURRING FLAVONOIDS [J].

BOHMONT, C ;

AARONSON, LM ;

MANN, K ;

PARDINI, RS .

JOURNAL OF NATURAL PRODUCTS, 1987, 50 (03) :427-433

[8] MITOCHONDRIAL GENERATION OF HYDROGEN-PEROXIDE - GENERAL PROPERTIES AND EFFECT OF HYPERBARIC-OXYGEN [J].

BOVERIS, A ;

CHANCE, B .

BIOCHEMICAL JOURNAL, 1973, 134 (03) :707-716

[9] The ATP synthase - A splendid molecular machine [J].

Boyer, PD .

ANNUAL REVIEW OF BIOCHEMISTRY, 1997, 66 :717-749

[10] NITRIC-OXIDE REGULATES MITOCHONDRIAL RESPIRATION AND CELL FUNCTIONS BY INHIBITING CYTOCHROME-OXIDASE [J].

BROWN, GC .

FEBS LETTERS, 1995, 369 (2-3) :136-139

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