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补体损伤的分子本质。

Molecular nature of the complement lesion.

作者信息

Bhakdi S, Tranum-Jensen J

出版信息

Proc Natl Acad Sci U S A. 1978 Nov;75(11):5655-9. doi: 10.1073/pnas.75.11.5655.

Abstract

The principle molecular event leading to membrane perturbation by complement is the assembly of the terminal five serum complement components (C5b-C9) into a macromolecular C5b-9 complex on the target membrane [Müller-Eberhard, H.-J. (1975) Ann. Rev. Biochem. 44, 697--723]. The present communication reports on the ability of purified C5b-9 complexes isolated from target membranes to become reincorporated into artificial lipid vesicles. The data indicate that the complex is a vertically oriented, hollow, cylindrical macromolecule possessing lipid-binding regions that enable one terminus to penetrate into the lipid bilayer. A transmembrane pore appears to be created at the attachment site of the C5b-9 complex.

摘要

补体导致膜扰动的主要分子事件是末端五个血清补体成分(C5b - C9)在靶膜上组装成大分子C5b - 9复合物[Müller - Eberhard, H.-J. (1975) Ann. Rev. Biochem. 44, 697 - 723]。本通讯报道了从靶膜分离的纯化C5b - 9复合物重新掺入人工脂质囊泡的能力。数据表明,该复合物是一个垂直取向的、中空的圆柱形大分子,具有脂质结合区域,使一端能够穿透脂质双层。在C5b - 9复合物的附着位点似乎形成了一个跨膜孔。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/71c5/393026/5a21ce91afd6/pnas00021-0420-a.jpg

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