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人类主要组织相容性复合体相关Fc受体的晶体结构及免疫球蛋白G结合特性(,)

Crystal structure and immunoglobulin G binding properties of the human major histocompatibility complex-related Fc receptor(,).

作者信息

West A P, Bjorkman P J

机构信息

Division of Biology 156-29 and Howard Hughes Medical Institute, California Institute of Technology, Pasadena, California 91125, USA.

出版信息

Biochemistry. 2000 Aug 15;39(32):9698-708. doi: 10.1021/bi000749m.

DOI:10.1021/bi000749m
PMID:10933786
Abstract

The neonatal Fc receptor (FcRn) performs two distinct but related functions: transport of maternal immunoglobulin G (IgG) to pre- or neonatal mammals, thus providing passive immunity, and protection of IgG from normal serum protein catabolism. FcRn is related to class I MHC proteins but lacks a functional peptide binding groove. The crystal structure of human FcRn has been determined at 2.7 A resolution and compared to the previously described structure of rat FcRn [Burmeister et al. (1994) Nature 372, 336-343] and to the structures of MHC and MHC-related proteins. Human FcRn is structurally similar to the rat receptor but does not form receptor dimers in the crystals as observed in crystals of rat FcRn. The interaction between human FcRn and IgG was characterized by determining the binding stoichiometry using equilibrium gel filtration and by deriving binding affinities for the different human IgG subclasses using a surface plasmon resonance assay. Like rat and mouse FcRn, human FcRn interacts with IgG with a 2:1 receptor:ligand stoichiometry. The binding of human FcRn to the four human IgG subclasses shows subclass and allotype variations but no clear subclass affinity differences that correlate with serum half-lives. The structure of human FcRn and studies of its ligand binding are relevant to current efforts to use FcRn-mediated regulation of IgG half-life in serum to increase the lifetimes of antibody-based therapeutics.

摘要

新生儿Fc受体(FcRn)具有两种不同但相关的功能:将母体免疫球蛋白G(IgG)转运至早产或新生哺乳动物,从而提供被动免疫,以及保护IgG免受正常血清蛋白分解代谢的影响。FcRn与I类主要组织相容性复合体(MHC)蛋白相关,但缺乏功能性肽结合槽。已确定人FcRn的晶体结构分辨率为2.7埃,并与先前描述的大鼠FcRn结构[Burmeister等人(1994年)《自然》372, 336 - 343]以及MHC和MHC相关蛋白的结构进行了比较。人FcRn在结构上与大鼠受体相似,但在晶体中不像大鼠FcRn晶体那样形成受体二聚体。通过使用平衡凝胶过滤确定结合化学计量,并使用表面等离子体共振分析得出不同人IgG亚类的结合亲和力,对人FcRn与IgG之间的相互作用进行了表征。与人FcRn与IgG的相互作用化学计量比为2:1。人FcRn与四种人IgG亚类的结合表现出亚类和同种异型差异,但没有与血清半衰期相关的明显亚类亲和力差异。人FcRn的结构及其配体结合研究与当前利用FcRn介导的血清中IgG半衰期调节来延长基于抗体的治疗药物寿命的努力相关。

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