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p25前序列肽与蜂毒肽的比较。红细胞溶血和带3聚集。

Comparison of p25 presequence peptide and melittin. Red blood cell haemolysis and band 3 aggregation.

作者信息

Clague M J, Cherry R J

机构信息

Department of Chemistry and Biological Chemistry, University of Essex, Colchester, U.K.

出版信息

Biochem J. 1988 Jun 15;252(3):791-4. doi: 10.1042/bj2520791.

Abstract

The 25 residue presequence (p25) for subunit IV of yeast cytochrome oxidase had previously been shown to possess structural and behavioural characteristics in common with the bee venom polypeptide, melittin. The present study extends the results of leakage experiments on model-membrane systems to the haemolysis of human erythrocytes, which both peptides are shown to accomplish in a manner sensitive to membrane potential. In addition, the laser flash-induced transient dichroism technique for measuring protein rotational diffusion has been used to show that both peptides aggregate band 3, the major integral membrane protein of the erythrocyte. Aggregation cannot be reversed by high ionic strength; this serves to differentiate these peptides from other positively charged species such as polylysine that aggregate band 3 at low ionic strength. These results suggest that aggregation of membrane proteins may possibly prove to be a feature of the interaction of p25 signal peptide with mitochondrial membranes.

摘要

酵母细胞色素氧化酶亚基IV的25个氨基酸残基的前导序列(p25)先前已被证明具有与蜂毒多肽蜂毒素相同的结构和行为特征。本研究将模型膜系统的泄漏实验结果扩展到了人红细胞的溶血实验,结果表明这两种肽都以对膜电位敏感的方式引起溶血。此外,用于测量蛋白质旋转扩散的激光闪光诱导瞬态二色性技术已被用于表明这两种肽都会聚集红细胞的主要整合膜蛋白带3。高离子强度不能逆转聚集;这有助于将这些肽与其他带正电荷的物质区分开来,例如在低离子强度下聚集带3的聚赖氨酸。这些结果表明,膜蛋白的聚集可能是p25信号肽与线粒体膜相互作用的一个特征。

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