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备解素、补体第三成分(C3)及其生理激活产物之间的相互作用分析。

Analysis of the interactions between properdin, the third component of complement (C3), and its physiological activation products.

作者信息

Farries T C, Lachmann P J, Harrison R A

机构信息

Mechanisms in Tumour Immunity Unit, MRC Centre, Cambridge, U.K.

出版信息

Biochem J. 1988 May 15;252(1):47-54. doi: 10.1042/bj2520047.

Abstract

The interactions of properdin with both surface-bound and fluid-phase C3 (the third component of complement) and its activation products have been investigated by using a purified preparation of the 'native' form. At physiological ionic strength, a weak interaction with cell-bound C3b (the larger activation fragment of C3) could be demonstrated. In the presence of Factor B this interaction was enhanced, and further enhancement was seen when C3bBb sites were formed on the erythrocytes. The avidities of properdin for cell-bound iC3b (the initial product of Factors I and H action on C3b) and C3b were compared at low ionic strength, with that measured for iC3b being less than that for C3b. In contrast, the affinities of properdin for fluid-phase C3b, iC3b and C3c (the larger product of Factors I and H or CR1 (the C3b receptor) action on iC3b) were all very similar, and apparently much weaker than that for cell-bound C3b. No interaction with either native C3 or, more surprisingly, C3i (haemolytically inactive C3) could be detected. Properdin also inhibited Factor I binding to, and action upon, cell-bound C3b, but did not inhibit Factor I action on fluid-phase C3b. These data permit a more detailed description of the roles of properdin in the alternative pathway of complement activation, emphasizing its importance in concentrating activation at the activating surface.

摘要

已使用“天然”形式的纯化制剂研究了备解素与表面结合的和液相的C3(补体第三成分)及其激活产物之间的相互作用。在生理离子强度下,可证明备解素与细胞结合的C3b(C3的较大激活片段)存在弱相互作用。在因子B存在的情况下,这种相互作用增强,当红细胞上形成C3bBb位点时,相互作用进一步增强。在低离子强度下比较了备解素对细胞结合的iC3b(因子I和H作用于C3b的初始产物)和C3b的亲和力,测得iC3b的亲和力低于C3b。相反,备解素对液相C3b、iC3b和C3c(因子I和H或CR1(C3b受体)作用于iC3b的较大产物)的亲和力都非常相似,且明显弱于对细胞结合的C3b的亲和力。未检测到备解素与天然C3或更令人惊讶的C3i(溶血无活性的C3)之间的相互作用。备解素还抑制因子I与细胞结合的C3b结合及其对细胞结合的C3b的作用,但不抑制因子I对液相C3b的作用。这些数据允许对备解素在补体激活替代途径中的作用进行更详细的描述,强调其在将激活集中于激活表面方面的重要性。

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