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对-(氯汞基)苯磺酸盐与膜蛋白的结合及对人红细胞水转运的抑制作用

p-(Chloromercuri)benzenesulfonate binding by membrane proteins and the inhibition of water transport in human erythrocytes.

作者信息

Benga G, Popescu O, Pop V I, Holmes R P

出版信息

Biochemistry. 1986 Apr 8;25(7):1535-8. doi: 10.1021/bi00355a011.

Abstract

The binding of [203Hg]-p-(chloromercuri)benzenesulfonate to the membrane proteins of human erythrocytes and erythrocyte ghosts was examined under conditions where binding to the bulk of membrane sulfhydryl groups was blocked by N-ethylmaleimide. Binding was essentially complete within 90 min when approximately 40 nmol was bound per milligram of membrane protein. This binding was correlated with the inhibition of water transport measured by an NMR technique. Maximal inhibition was observed with the binding of approximately 10 nmol of p-(chloromercuri)benzenesulfonate/mg of membrane protein. Under these conditions, both band 3 and band 4.5 bound 1 mol of inhibitor/mol of protein. In contrast to previous experiments, these results indicate that band 4.5 proteins as well as band 3 have to be considered as playing a role in water transport.

摘要

在通过N - 乙基马来酰亚胺阻断与大部分膜巯基结合的条件下,研究了[203Hg] - 对 - (氯汞基)苯磺酸盐与人红细胞及红细胞血影膜蛋白的结合情况。当每毫克膜蛋白结合约40 nmol时,结合在90分钟内基本完成。这种结合与通过核磁共振技术测量的水转运抑制相关。当每毫克膜蛋白结合约10 nmol对 - (氯汞基)苯磺酸盐时观察到最大抑制。在这些条件下,带3和带4.5蛋白每摩尔蛋白结合1摩尔抑制剂。与先前的实验不同,这些结果表明带4.5蛋白以及带3蛋白都必须被视为在水转运中起作用。

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