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防御素可促进带负电荷细胞膜的融合与裂解。

Defensins promote fusion and lysis of negatively charged membranes.

作者信息

Fujii G, Selsted M E, Eisenberg D

机构信息

Molecular Biology Institute, University of California, Los Angeles, 90024-1570.

出版信息

Protein Sci. 1993 Aug;2(8):1301-12. doi: 10.1002/pro.5560020813.

Abstract

Defensins, a family of cationic peptides isolated from mammalian granulocytes and believed to permeabilize membranes, were tested for their ability to cause fusion and lysis of liposomes. Unlike alpha-helical peptides whose lytic effects have been extensively studied, the defensins consist primarily of beta-sheet. Defensins fuse and lyse negatively charged liposomes but display reduced activity with neutral liposomes. These and other experiments suggest that fusion and lysis is mediated primarily by electrostatic forces and to a lesser extent, by hydrophobic interactions. Circular dichroism and fluorescence spectroscopy of native defensins indicate that the amphiphilic beta-sheet structure is maintained throughout the fusion process. Taken together, these results support the idea that protein-mediated membrane fusion depends not only on hydrophobic and electrostatic forces but also on the spatial arrangement of the amino acid residues to form a three-dimensional amphiphilic structure, which promotes the efficient mixing of the lipids between membranes. A molecular model for membrane fusion by defensins is presented, which takes into account the contributions of electrostatic forces, hydrophobic interactions, and structural amphiphilicity.

摘要

防御素是从哺乳动物粒细胞中分离出的一类阳离子肽,被认为可使细胞膜通透性增加,对其诱导脂质体融合和裂解的能力进行了测试。与已对其裂解作用进行广泛研究的α-螺旋肽不同,防御素主要由β-折叠组成。防御素可使带负电荷的脂质体融合并裂解,但对中性脂质体的活性降低。这些实验及其他实验表明,融合和裂解主要由静电力介导,在较小程度上由疏水相互作用介导。天然防御素的圆二色光谱和荧光光谱表明,两亲性β-折叠结构在整个融合过程中得以维持。综上所述,这些结果支持了这样一种观点,即蛋白质介导的膜融合不仅取决于疏水作用力和静电力,还取决于氨基酸残基的空间排列以形成三维两亲性结构,这种结构促进了膜间脂质的有效混合。本文提出了一个防御素介导膜融合的分子模型,该模型考虑了静电力、疏水相互作用和结构两亲性的作用。

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