Jarva H, Jokiranta T S, Hellwage J, Zipfel P F, Meri S
Department of Bacteriology, Haartman Institute, University of Helsinki, Finland.
J Immunol. 1999 Oct 1;163(7):3957-62.
C-reactive protein (CRP) is a major acute phase protein whose functions are not totally clear. In this study, we examined the interaction of CRP with factor H (FH), a key regulator of the alternative pathway (AP) of complement. Using the surface plasmon resonance technique and a panel of recombinantly expressed FH constructs, we observed that CRP binds to two closely located regions on short consensus repeat (SCR) domains 7 and 8-11 of FH. Also FH-like protein 1 (FHL-1), an alternatively spliced product of the FH gene, bound to CRP with its most C-terminal domain (SCR 7). The binding reactions were calcium-dependent and partially inhibited by heparin. In accordance with the finding that CRP binding sites on FH were distinct from the C3b binding sites, CRP preserved the ability of FH to promote factor I-mediated cleavage of C3b. We propose that the function of CRP is to target functionally active FH and FHL-1 to injured self tissues. Thereby, CRP could restrict excessive complement attack in tissues while allowing a temporarily enhanced AP activity against invading microbes in blood.
C反应蛋白(CRP)是一种主要的急性期蛋白,其功能尚不完全清楚。在本研究中,我们检测了CRP与补体替代途径(AP)的关键调节因子H因子(FH)之间的相互作用。使用表面等离子体共振技术和一组重组表达的FH构建体,我们观察到CRP与FH的短共识重复序列(SCR)结构域7以及8-11上两个紧密相邻的区域结合。此外,FH样蛋白1(FHL-1)是FH基因的可变剪接产物,其最末端结构域(SCR 7)与CRP结合。结合反应依赖于钙,并部分受到肝素的抑制。鉴于CRP在FH上的结合位点与C3b结合位点不同,CRP保留了FH促进I因子介导的C3b裂解的能力。我们提出,CRP的功能是将具有功能活性的FH和FHL-1靶向受损的自身组织。因此,CRP可以限制组织中补体的过度攻击,同时允许血液中针对入侵微生物的替代途径活性暂时增强。
