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The immunoglobulin heavy chain constant region affects kinetic and thermodynamic parameters of antibody variable region interactions with antigen

机译:免疫球蛋白重链恒定区影响抗体可变区与抗原相互作用的动力学和热力学参数

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摘要

A central dogma in immunology is that antibody specificity is a function of the variable (V) region. However serological analysis of IgG(1), IgG(2a), and IgG(2b) switch variants of murine monoclonal antibody (mAb) 3E5 IgG(3) with identical V domains revealed apparent specificity differences for Cryptococcus neoformans glucuronoxylomannan (GXM). Kinetic and thermodynamic binding properties of mAbs 3E5 to a 12-mer peptide mimetic of GXM revealed differences in the affinity of these mAbs for a monovalent ligand, a result that implied that the constant (C) region affects the secondary structure of the antigen binding site, thus accounting for variations in specificity. Structural models of mAbs 3E5 suggested that isotype-related differences in binding resulted from amino acid sequence polymorphisms in the C region. This study implies that isotype switching is another mechanism for generating diversity in antigen binding and that isotype restriction of certain antibody responses may reflect structural constraints imposed by C region on V region binding. Furthermore, isotype affected the polyreactivity of V region identical antibodies, implying a role for C region in determining self-reactivity.
机译:免疫学的中心教条是抗体特异性是可变(V)区的函数。但是,对具有相同V结构域的鼠单克隆抗体(mAb)3E5 IgG(3)的IgG(1),IgG(2a)和IgG(2b)开关变体进行血清学分析,发现新隐球菌葡糖醛酸甘露聚糖(GXM)有明显的特异性差异。 mAbs 3E5与GXM的12-mer肽模拟物的动力学和热力学结合特性表明,这些mAb对单价配体的亲和力存在差异,结果表明恒定(C)区会影响抗原结合位点的二级结构,从而说明了特异性的差异。 mAbs 3E5的结构模型表明,结合的同种型相关差异是由C区的氨基酸序列多态性引起的。该研究表明同种型转换是在抗原结合中产生多样性的另一种机制,某些抗体应答的同种型限制可能反映了C区对V区结合施加的结构限制。此外,同种型影响V区相同抗体的多反应性,暗示C区在确定自身反应性中的作用。

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