Core Research Laboratory, The Second Affiliated Hospital, Xi'an Jiaotong University, Xi'an, Shaanxi, China.
J Immunol Res. 2017;2017:8193932. doi: 10.1155/2017/8193932. Epub 2017 Jun 15.
After the discovery of the C5a receptor C5aR1, C5aR2 is the second receptor found to bind C5a and its des-arginine form. As a heptahelical G protein-coupled receptor but devoid of the intracellular G signal, C5aR2 is special and confusing. Ramifications and controversies about C5aR2 are under debate since its identification, from putative ligands and cellular localization to intracellular signals and pathological roles in inflammation and immunity. The ruleless and even conflicting pro- or anti-inflammatory role of C5aR2 in animal models of diverse diseases makes one bewildered. This review summarizes reports on C5aR2, tries to clear up available evidence on these four controversial aspects, and delineates C5aR2 function(s). It also summarizes available toolboxes for C5aR2 study.
C5a 受体 C5aR1 发现后,C5aR2 是第二个被发现能结合 C5a 及其去精氨酸形式的受体。作为一种七螺旋 G 蛋白偶联受体,但缺乏细胞内 G 信号,C5aR2 是特殊且令人困惑的。自其鉴定以来,关于 C5aR2 的分支和争议一直在争论中,从假定的配体和细胞定位到细胞内信号以及在炎症和免疫中的病理作用。C5aR2 在不同疾病动物模型中的无规则甚至相互矛盾的促炎或抗炎作用让人感到困惑。这篇综述总结了关于 C5aR2 的报告,试图澄清这四个有争议方面的现有证据,并描绘 C5aR2 的功能。它还总结了用于 C5aR2 研究的现有工具箱。
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