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巨噬细胞补体受体与病原体清除

Macrophage complement receptors and pathogen clearance.

作者信息

van Lookeren Campagne Menno, Wiesmann Christian, Brown Eric J

机构信息

Department of Immunology, Genentech, 1 DNA Way, South San Francisco, CA 94080, USA.

出版信息

Cell Microbiol. 2007 Sep;9(9):2095-102. doi: 10.1111/j.1462-5822.2007.00981.x. Epub 2007 Jun 21.

Abstract

Phagocytosis, an important mechanism of the host-defence system and a primary function of macrophages, is facilitated by opsonization, a process by which serum components tag pathogens for recognition by neutrophils and macrophages. Complement component C3 is central to opsonization. Its first cleavage product, C3b, forms the multisubunit enzyme, C3bBb, which proteolytically cleaves additional C3 molecules on the pathogen surface. C3b is further degraded to iC3b, C3c and C3dg, products that serve as ligands for selective complement receptors on leukocytes. This receptor-ligand interaction subsequently modulates immune responses or directly targets the pathogen for clearance by phagocytosis. Although a central role for C3 in phagocytosis of certain pathogens is well accepted, the receptors orchestrating the phagocytic response have not been well characterized. The recent structures of C3 and its breakdown products have increased our insights into the molecular basis of complement activation and recognition by their receptors. Here we review the biology of macrophage receptors for C3 fragments and discuss their role in the host response to pathogens.

摘要

吞噬作用是宿主防御系统的重要机制,也是巨噬细胞的主要功能,它通过调理作用得以促进,调理作用是血清成分标记病原体以便被中性粒细胞和巨噬细胞识别的过程。补体成分C3是调理作用的核心。其首个裂解产物C3b形成多亚基酶C3bBb,该酶可在病原体表面蛋白水解裂解其他C3分子。C3b进一步降解为iC3b、C3c和C3dg,这些产物作为白细胞上选择性补体受体的配体。这种受体-配体相互作用随后调节免疫反应或直接靶向病原体以便通过吞噬作用清除。尽管C3在某些病原体吞噬作用中的核心作用已被广泛接受,但协调吞噬反应的受体尚未得到很好的表征。C3及其分解产物的最新结构增加了我们对补体激活及其受体识别的分子基础的认识。在这里,我们综述了巨噬细胞C3片段受体的生物学特性,并讨论了它们在宿主对病原体反应中的作用。

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