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糖基化缺失的 IgG1 抗体通过提高与 FcγR 的结合能力而获得效应功能。

Avidity confers FcγR binding and immune effector function to aglycosylated immunoglobulin G1.

机构信息

Biologics Research, Centocor R&D Inc., Radnor, PA 19087, USA.

出版信息

J Mol Recognit. 2012 Mar;25(3):147-54. doi: 10.1002/jmr.2155.

DOI:10.1002/jmr.2155
PMID:22407978
Abstract

Immunoglobulin G (IgG) antibodies are an integral part of the adaptive immune response that provide a direct link between humoral and cellular components of the immune system. Insights into relationships between the structure and function of human IgGs have prompted molecular engineering efforts to enhance or eliminate specific properties, such as Fc-mediated immune effector functions. Human IgGs have an N-glycosylation site at Asn297, located in the second heavy chain constant region (CH2). The composition of the Fc glycan can have substantial impacts on Fc gamma receptor(FcγR) binding. The removal of the glycan through enzymatic deglycosylation or mutagenesis of the N-linked glycosylation site has been reported to "silence" FcγR-binding and effector functions, particularly with assays that measure monomeric binding. However, interactions between IgGs and FcγRs are not limited to monomeric interactions but can be influenced by avidity, which takes into account the sum of multimeric interactions between antigen-engaged IgGs and FcγRs. We show here that under in vitro conditions, which allowed avidity binding, aglycosylated IgGs can bind to one of the FcγRs, FcγRI, and mediate effector functions. These studies highlight how the valency of a molecular interaction (monomeric binding versus avidity binding) can influence antibody/FcγR interactions such that avidity effects can translate very low intrinsic affinities into significant functional outcomes.

摘要

免疫球蛋白 G(IgG)抗体是适应性免疫反应的一个组成部分,它在免疫系统的体液和细胞成分之间提供了直接的联系。对人类 IgG 结构和功能之间关系的深入了解促使人们进行分子工程努力,以增强或消除特定的特性,如 Fc 介导的免疫效应功能。人类 IgG 在位于第二重链恒定区(CH2)的 Asn297 处具有 N-糖基化位点。Fc 聚糖的组成可以对 FcγR(FcγR)结合产生重大影响。通过酶促去糖基化或 N 连接糖基化位点的突变去除聚糖已被报道可以“沉默”FcγR 结合和效应功能,特别是在测量单体结合的测定中。然而,IgG 与 FcγR 之间的相互作用不仅限于单体相互作用,还可以受到亲和性的影响,亲和性考虑了抗原结合的 IgG 与 FcγR 之间多聚体相互作用的总和。我们在这里表明,在允许亲和性结合的体外条件下,糖基化的 IgG 可以与 FcγR 之一 FcγRI 结合并介导效应功能。这些研究强调了分子相互作用的价数(单体结合与亲和性结合)如何影响抗体/FcγR 相互作用,使得亲和性效应可以将非常低的固有亲和力转化为显著的功能结果。

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