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氧化应激期间碳酸酐酶III上巯基的S-硫醇化和不可逆氧化:一种研究完整细胞和组织中蛋白质修饰的方法。

S-thiolation and irreversible oxidation of sulfhydryls on carbonic anhydrase III during oxidative stress: a method for studying protein modification in intact cells and tissues.

作者信息

Lii C K, Chai Y C, Zhao W, Thomas J A, Hendrich S

机构信息

Department of Food Science and Human Nutrition, Iowa State University, Ames 50011.

出版信息

Arch Biochem Biophys. 1994 Jan;308(1):231-9. doi: 10.1006/abbi.1994.1033.

Abstract

S-thiolation of carbonic anhydrase III (CA III) in cultured rat hepatocytes under oxidative stress was studied by immunodetection on nitrocellulose blots of isoelectrofocusing gels. In cells treated with menadione, three S-thiolated forms of CA III were detected, whereas only two forms were observed in hepatocytes treated with t-butyl hydroperoxide. Two "nonreducible" oxidized forms of CA III were also detected on nitrocellulose blots. These forms increased with the amount of stress and were the only modified forms of CA III in buthionine sulfoxide-treated hepatocytes containing 10-fold less glutathione than control hepatocytes. These experiments support the concept that S-thiolation protects CA III from irreversible oxidation during oxidative stress. Partly and fully S-thiolated forms of CA III were easily detected in both male and female hepatocytes by the immunoblotting method, although female cells contained 15-fold less CA III than did male liver. S-thiolated forms of CA III were also detected in rat skeletal muscle and heart showing the utility of this method for determining the effect of oxidative stress on specific S-thiolatable protein in several tissues in vivo.

摘要

通过对等电聚焦凝胶的硝酸纤维素印迹进行免疫检测,研究了氧化应激条件下培养的大鼠肝细胞中碳酸酐酶III(CA III)的S-硫醇化情况。在用甲萘醌处理的细胞中,检测到三种CA III的S-硫醇化形式,而在用叔丁基过氧化氢处理的肝细胞中仅观察到两种形式。在硝酸纤维素印迹上还检测到两种“不可还原”的CA III氧化形式。这些形式随着应激量的增加而增加,并且是在谷胱甘肽含量比对照肝细胞少10倍的丁硫氨酸亚砜处理的肝细胞中CA III的唯一修饰形式。这些实验支持了S-硫醇化在氧化应激期间保护CA III免受不可逆氧化的概念。通过免疫印迹法在雄性和雌性肝细胞中都很容易检测到部分和完全S-硫醇化形式的CA III,尽管雌性细胞中的CA III含量比雄性肝脏少15倍。在大鼠骨骼肌和心脏中也检测到了CA III的S-硫醇化形式,这表明该方法可用于确定氧化应激对体内多个组织中特定可S-硫醇化蛋白的影响。

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