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补体对有核细胞的杀伤作用:C5b-9通道大小和细胞外Ca2+对溶解过程的影响。

Nucleated cell killing by complement: effects of C5b-9 channel size and extracellular Ca2+ on the lytic process.

作者信息

Kim S H, Carney D F, Hammer C H, Shin M L

出版信息

J Immunol. 1987 Mar 1;138(5):1530-6.

PMID:2433349
Abstract

For C5b-9 channels to mediate cytolysis of a nucleated cell, a sufficient number of channels must be formed in the plasma membrane to override the compensatory mechanisms that nucleated cells might employ to survive. It is well known that nucleated cells are relatively resistant to lysis by complement in comparison to erythrocytes, and it is now evident that this resistance is due, in part, to the ability of nucleated cells to rapidly eliminate C5b-9 from the cell surface. The ability of nucleated cells to eliminate complement complexes is related to physiochemical properties of the complex, such as channel diameter, which in turn affect Ca2+ fluxes that stimulate metabolic processes involved in the elimination process. Paradoxically, these same channel properties that stimulate the defense response may also be responsible for the lethal effects of complement. To further study the role of channel size on cytolysis of nucleated cells by C5b-9, we examined the lytic efficiency of larger C5b-9 channels containing several C9 molecules in comparison with smaller C5b-9 channels containing fewer C9. We have obtained data to indicate that although the larger channels were more cytolytically potent, the channel size had little influence on the rate of cell death. In contrast, the rate of lysis of erythrocytes was substantially slower when smaller C5b-9 channels were present. In evaluating the effect of the extracellular Ca2+ concentration, [Ca2+]o, on nucleated cell lysis in the presence of a lytic number of C5b-9 complexes, it was observed that when the [Ca2+]o was increased the rate of cell death also increased. These findings suggest that lysis of nucleated cells by C5b-9, unlike erythrocytes, may not be entirely due to colloid osmotic deregulation.

摘要

为使C5b - 9通道介导有核细胞的细胞溶解,必须在质膜中形成足够数量的通道,以克服有核细胞可能用于存活的补偿机制。众所周知,与红细胞相比,有核细胞对补体介导的溶解相对具有抗性,现在很明显这种抗性部分归因于有核细胞从细胞表面快速清除C5b - 9的能力。有核细胞清除补体复合物的能力与复合物的物理化学性质有关,如通道直径,而通道直径又会影响Ca2 +通量,进而刺激参与清除过程的代谢过程。矛盾的是,这些刺激防御反应的相同通道特性也可能是补体致死效应的原因。为了进一步研究通道大小对C5b - 9介导的有核细胞溶解的作用,我们比较了含有多个C9分子的较大C5b - 9通道与含有较少C9分子的较小C5b - 9通道的溶解效率。我们获得的数据表明,尽管较大的通道在细胞溶解方面更具效力,但通道大小对细胞死亡速率影响很小。相反,当存在较小的C5b - 9通道时,红细胞的溶解速率要慢得多。在评估细胞外Ca2 +浓度[Ca2 +]o对存在溶解数量的C5b - 9复合物时的有核细胞溶解的影响时,观察到当[Ca2 +]o增加时,细胞死亡速率也增加。这些发现表明,与红细胞不同,C5b - 9介导的有核细胞溶解可能并不完全归因于胶体渗透压失调。

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