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The mechanism of pore assembly for a cholesterol-dependent cytolysin: formation of a large prepore complex precedes the insertion of the transmembrane beta-hairpins.

机译:胆固醇依赖性溶血素的孔组装机制:大的前孔复合物的形成先于跨膜β-发夹的插入。

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摘要

Perfringolysin O (PFO) is a member of the cholesterol-dependent cytolysin (CDC) family of membrane-penetrating toxins. The CDCs form large homooligomers (estimated to be comprised of up to 50 CDC monomers) that are responsible for generating a large pore in cholesterol-containing membranes of eukaryotic cells. The assembly of the PFO cytolytic complex was examined to determine whether it forms an oligomeric prepore complex on the membrane prior to the insertion of its membrane-spanning beta-sheet. A PFO oligomeric complex was formed on liposomes at both 4 degrees C and 37 degrees C and shown by SDS-agarose gel electrophoresis to be comprised of a large, comparatively homogeneous complex instead of a distribution of oligomer sizes. At low temperature, the processes of oligomerization and membrane insertion could be resolved, and PFO was found to form an oligomer without significant membrane insertion of its beta-hairpins. Furthermore, PFO was found to increase the ion conductivity through a planar bilayer by large and discrete stepwise changes in conductance that are consistent with the insertion of a preassembled pore complex into the bilayer. The combined results of these analyses strongly support the hypothesis that PFO forms a large oligomeric prepore complex on the membrane surface prior to the insertion of its transmembrane beta-sheet.
机译:Perfringolysin O(PFO)是膜穿透毒素的胆固醇依赖性细胞溶素(CDC)家族的成员。 CDC形成大的均聚物(估计由多达50个CDC单体组成),负责在含胆固醇的真核细胞膜中产生大孔。检查PFO溶细胞复合物的组装,以确定在插入跨膜β-折叠层之前是否在膜上形成寡聚前孔复合物。 PFO低聚复合物在4摄氏度和37摄氏度下均在脂质体上形成,并通过SDS-琼脂糖凝胶电泳显示其由较大的,相对均一的复合物组成,而不是由低聚物大小的分布所组成。在低温下,低聚和膜插入的过程可以解决,并且发现PFO形成了低聚物,而其β-发夹没有明显的膜插入。此外,发现PFO通过电导的大而离散的逐步变化来增加通过平面双层的离子电导率,这与将预组装的孔配合物插入双层一致。这些分析的综合结果强有力地支持了以下假设:PFO在插入其跨膜β-折叠层之前在膜表面形成了一个大的寡聚前孔复合体。

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