CYTOSOLIC FREE CA2+ AND PROTEOLYSIS IN LETHAL OXIDATIVE INJURY IN ENDOTHELIAL-CELLS

被引：109

作者：

GEERAERTS, MD

RONVEAUXDUPAL, MF

LEMASTERS, JJ

HERMAN, B

机构：

[1] UNIV N CAROLINA, SCH MED,DEPT CELL BIOL & ANAT,CELL BIOL LABS, CAMPUS BOX 7090,232 TAYLOR BLDG, CHAPEL HILL, NC 27599 USA

[2] FAC UNIV NAMUR, UNITE CYTOL, B-5000 NAMUR, BELGIUM

来源：

AMERICAN JOURNAL OF PHYSIOLOGY | 1991年 / 261卷 / 05期

关键词：

PROTEASE; LEUPEPTIN; PEPSTATIN; CALCIUM; PH; ENDOTHELIAL CELL; TOXIC OXYGEN SPECIES; OXIDATIVE STRESS;

D O I：

10.1152/ajpcell.1991.261.5.C889

中图分类号：

Q4 [生理学];

学科分类号：

071003 ;

摘要：

Oxygen free radicals (OFR) are thought to mediate ischemia-reperfusion injury to endothelium of heart, lung, brain, liver, and kidney and contribute to development of atherosclerosis, pulmonary O2 toxicity, and adult respiratory distress syndrome. Increased cytosolic free Ca2+ (Ca(i)2+) has been proposed as a mechanism of injury from oxidative stress, yet the pathways by which an increase in Ca(i)2+ may cause OFR-mediated endothelial cell injury remain unknown. Using multiparameter digitized video microscopy and the fluorescent probes, fura-2 acetoxymethyl ester and propidium iodide, we measured Ca(i)2+ and cell viability in human umbilical endothelial cells during oxidative stress with xanthine (50-mu-M) plus xanthine oxidase (40 mU/ml). Oxidative stress caused a sustained increase in Ca(i)2+ from a resting level of 90-100 nM to near 500 nM, which was preceded by formation of plasma membrane blebs. The increase in Ca(i)2+ was prevented by removal of extracellular Ca2+ (Ca(o)2+). Prevention of the increase in Ca(i)2+ was associated with prolonged cell viability. Readdition of Ca(o)2+ resulted in an immediate large increase in Ca(i)2+ and rapid onset of cell death. The protease inhibitors, leupeptin and pepstatin, delayed the increase in Ca(i)2+ and prolonged cell viability. The results are consistent with the hypothesis that endothelial cell injury due to oxidative stress may be the result of Ca(i)2+ influx and resultant activation of Ca2+-dependent proteases.

引用

页码：C889 / C896

页数：8

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