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细胞结合的C3片段增强C56启动的溶解作用:一种独立于C56与C3b预先结合的机制的证据。

Enhancement of C56-initiated lysis by cell-bound C3 fragments: evidence for a mechanism independent of the prior binding of C56 to C3b.

作者信息

Yamamoto K I, Lint T F, Gewurz H

出版信息

J Immunol. 1977 Oct;119(4):1346-50.

PMID:894040
Abstract

Cell-bound C3b can reversibly bind C56, the activated complex of the fifth (C5) and sixth (C6) components of complement, and in this way potentiate C56-initiated lysis by favoring the formation of C567 at the cell surface. We report here another way in which cell-bound C3 fragments can enhance C56-initiated lysis, which involves C567 generated in the fluid phase rather than at the cell surface. Evidence for the involvement of fluid phase C567 was obtained by use of dextran sulfate, which is known to inhibit the hemolysis of E mediated by fluid phase C567. Dextran sulfate strongly inhibited the formation of C567 sites on cells bearing C4b and C3b (EAC4b3b) as well as on unmodified E when C56 and C7 were added simultaneously to the cells. By contrast, dextran sulfate had virtually no effect on the reaction sequence involving the prior binding of C56 to C3b and subsequent formation of C567 at the cell surface. Treatment of EAC4b3b with either anti-C3 Fab' fragments or the C3b inactivator reduced but did not eliminate the enhancement of hemolysis, raising the possibilities that a C3 fragment(s) other than C3b also can enhance C56-initiated lysis and/or that the enhancement is indirect without a requirement for an interaction between C567 and the cell-bound C3 fragment itself.

摘要

结合在细胞上的C3b能够可逆地结合补体第五(C5)和第六(C6)成分的活化复合物C56,并通过促进细胞表面C567的形成,以这种方式增强由C56启动的细胞溶解。我们在此报告结合在细胞上的C3片段增强C56启动的细胞溶解的另一种方式,这涉及在液相而非细胞表面产生的C567。通过使用硫酸葡聚糖获得了液相C567参与的证据,已知硫酸葡聚糖可抑制由液相C567介导的E的溶血。当将C56和C7同时添加到细胞中时,硫酸葡聚糖强烈抑制了在带有C4b和C3b的细胞(EAC4b3b)以及未修饰的E上C567位点的形成。相比之下,硫酸葡聚糖对涉及C56先与C3b结合并随后在细胞表面形成C567的反应序列几乎没有影响。用抗C3 Fab'片段或C3b灭活剂处理EAC4b3b可降低但不能消除溶血增强,这增加了除C3b之外的其他C3片段也可增强C56启动的细胞溶解和/或增强是间接的且不需要C567与结合在细胞上的C3片段本身之间相互作用的可能性。

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