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补体C5b-9膜损伤处溶质扩散分析:单个C5b-9复合物并非作为离散、均匀的孔发挥作用的证据。

Analysis of solute diffusion across the C5b-9 membrane lesion of complement: evidence that individual C5b-9 complexes do not function as discrete, uniform pores.

作者信息

Sims P J, Lauf P K

出版信息

J Immunol. 1980 Dec;125(6):2617-25.

PMID:7430641
Abstract

We have investigated the diffusion of radiolabeled nonelectrolytes across the membranes of resealed erythrocyte ghosts that had been treated with the terminal complement components C5b-9 and incubated under nonlytic steady state conditions. For all solutes tested, we note that diffusion across the C5b-9 lesion is retarded to rates more than 2 orders of magnitude slower than can be anticipated for a transmembrane diffusional channel of the dimensions suggested by the ultrastructure of the C5b-9 membrane lesion. Furthermore, direct measurement of the relative selectivity of the C5b-9 membrane lesions to permeation by solutes of differing molecular radii suggests that individual membrane lesions are not of uniform functional size. Data are presented that suggest that the functional heterogeneity of the membrane lesion is due to the aggregation of individual membrane bound C5b-9 complexes into larger functional units and not due to variable stoichiometry of C9 within the individual C5b-9 complex.

摘要

我们研究了放射性标记的非电解质在经末端补体成分C5b-9处理并在非溶解稳态条件下孵育的重封红细胞膜囊泡膜上的扩散情况。对于所有测试的溶质,我们注意到跨C5b-9损伤的扩散受到阻碍,其速率比根据C5b-9膜损伤超微结构所提示尺寸的跨膜扩散通道预期速率慢2个数量级以上。此外,对C5b-9膜损伤对不同分子半径溶质渗透的相对选择性的直接测量表明,单个膜损伤的功能大小并不均匀。所呈现的数据表明,膜损伤的功能异质性是由于单个膜结合的C5b-9复合物聚集成更大的功能单位,而不是由于单个C5b-9复合物内C9的化学计量比不同。

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