SEVERAL NONGENOTOXIC CARCINOGENS UNCOUPLE MITOCHONDRIAL OXIDATIVE-PHOSPHORYLATION

被引：14

作者：

KELLER, BJ

MARSMAN, DS

POPP, JA

THURMAN, RG

机构：

[1] UNIV N CAROLINA, DEPT PHARMACOL,HEPATOBIOL & TOXICOL LAB,CB 7365, FAC LAB OFF BLDG, CHAPEL HILL, NC 27599 USA

[2] CHEM IND INST TOXICOL, RES TRIANGLE PK, NC 27709 USA

来源：

BIOCHIMICA ET BIOPHYSICA ACTA | 1992年 / 1102卷 / 02期

关键词：

OXIDATIVE PHOSPHORYLATION; MITOCHONDRION; NONGENOTOXIC CARCINOGEN; LIVER; PEROXISOMAL PROLIFERATOR; (RAT);

D O I：

10.1016/0005-2728(92)90105-B

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

A number of plasticizers and lipid-lowering drugs induce peroxisomes and cause hepatocellular carcinoma in rodents by mechanisms which remain unknown. In this study, seven structurally dissimilar peroxisome proliferating agents were shown to uncouple oxidative phosphorylation in isolated rat liver mitochondria. For example, perfluorooctanoate (0.5 mM) increased succinate-induced (state 4) mitochondrial respiration by over 50% while stimulation of state 3 respiration with ADP was minimal (i.e., uncoupling occurred). Interestingly, compounds which are potent carcinogens in vivo (e.g., Wy-14,643 and perfluorooctanoate) were more powerful uncouplers of oxidative phosphorylation in vitro than weak tumor-causing agents (e.g., valproate). Uncoupling also occurred in vivo. Basal rates of oxygen uptake in perfused livers from chronically treated rats were increased from 137 +/- 7 mumol g-1/h in pair-fed controls to 153 +/- 5 mumol g-1/h after 2.5 months of feeding Wy-14,643 (0.1% w/v in diet). Concomitantly, rates of urea synthesis from ammonia, a process highly dependent on ATP supply, were reduced almost completely from 104 +/- 10 mumol g-1/h to 13 +/- 6 mumol g-1/h. Bile flow, another energy-dependent process, was also reduced significantly by treatment with Wy-14,643 in vivo for 24 h. Taken together, these data indicate that energy supply for cellular processes such as urea synthesis and bile flow was disrupted in vivo due to uncoupling of oxidative phosphorylation by Wy-14,643. It is proposed that peroxisomal proliferators accumulate in the liver where they uncouple mitochondrial oxidative phosphorylation and interfere with cellular energetics.

引用

页码：237 / 244

页数：8

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