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Soluble human complement receptor type 1 inhibits complement-mediated host defense.

机译:1型可溶性人类补体受体抑制补体介导的宿主防御。

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摘要

Soluble complement receptor type 1 (sCR1) is a powerful inhibitor of complement activation. Because of this ability, sCR1 may prove to be an important therapeutic agent that can be used to block the immunopathologic effects of uncontrolled complement activation in a variety of clinically significant disorders. Although several previous studies have examined the ability of sCR1 to inhibit complemented-mediated immunopathologic damage, there is no information on its ability to interfere with the host's defense against infection. In the current experiments sCR1 exerted a concentration-dependent inhibitory effect on the phagocytosis of Streptococcus pneumoniae by human polymorphonuclear leukocytes in vitro. Not only di sCR1 inhibit complement-dependent opsonization of the pneumococcus but at higher concentrations it also inhibited the ingestion of bacteria which had been previously opsonized. Furthermore, when rats were injected with sCR1, it inhibited both their serum hemolytic activity and serum opsonic activity in a dose-dependent fashion. Finally, for rats treated with sCR1, the 50% lethal dose was S. pneumoniae and Pseudomonas aeruginosa. These data demonstrate that sCR1 significantly inhibits complement-mediated host against bacterial infection.
机译:1型可溶性补体受体(sCR1)是补体激活的强大抑制剂。由于这种能力,sCR1可能被证明是一种重要的治疗剂,可用于阻断多种临床意义重大疾病中不受控制的补体激活的免疫病理作用。尽管先前的一些研究已经检查了sCR1抑制补体介导的免疫病理损伤的能力,但尚无关于其干扰宿主抗感染防御能力的信息。在当前的实验中,sCR1对人多形核白细胞在体外对肺炎链球菌的吞噬作用具有浓度依赖性的抑制作用。 di sCR1不仅抑制肺炎球菌的补体依赖性调理作用,而且在更高的浓度下,还抑制了先前调理过的细菌的摄入。此外,当给大鼠注射sCR1时,它会以剂量依赖性方式抑制其血清溶血活性和血清调理活性。最后,对于用sCR1治疗的大鼠,其50%致死剂量为肺炎链球菌和铜绿假单胞菌。这些数据表明,sCR1显着抑制补体介导的宿主抵抗细菌感染。

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