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Allosteric Effects between the Antibody Constant and Variable Regions: A Study of IgA Fc Mutations on Antigen Binding

机译:抗体恒定区和可变区之间的变构效应:IgA Fc突变对抗原结合的研究

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摘要

Therapeutic antibodies have shifted the paradigm of disease treatments from small molecules to biologics, especially in cancer therapy. Despite the increasing number of antibody candidates, much remains unknown about the antibody and how its various regions interact. Recent findings showed that the antibody constant region can govern localization effects that are useful in reducing side effects due to systemic circulation by the commonly used IgG isotypes. Given their localized mucosal effects, IgA antibodies are increasingly promising therapeutic biologics. While the antibody Fc effector cell activity has been a focus point, recent research showed that the Fc could also influence antigen binding, challenging the conventional idea of region-specific antibody functions. To investigate this, we analysed the IgA antibody constant region and its distal effects on the antigen binding regions using recombinant Pertuzumab IgA1 and IgA2 variants. We found that mutations in the C-region reduced Her2 binding experimentally, and computational structural analysis showed that allosteric communications were highly dependent on the antibody hinge, providing strong evidence that we should consider antibodies as whole proteins rather than a sum of functional regions.
机译:治疗性抗体已将疾病治疗的范式从小分子转变为生物制剂,尤其是在癌症治疗中。尽管候选抗体的数量在增加,但是关于抗体及其不同区域如何相互作用仍知之甚少。最近的发现表明,抗体恒定区可以控制定位作用,该作用可用于减少由于常用的IgG同种型引起的全身循环引起的副作用。鉴于其局部粘膜作用,IgA抗体正日益成为有希望的治疗生物制剂。尽管抗体Fc效应细胞的活性一直是重点,但最近的研究表明Fc也可能影响抗原结合,挑战了区域特异性抗体功能的传统观念。为了对此进行研究,我们使用重组帕妥珠单抗IgA1和IgA2变体分析了IgA抗体恒定区及其对抗原结合区的远端作用。我们发现,C区域的突变实验性地降低了Her2的结合,并且计算结构分析表明,变构通讯高度依赖于抗体铰链,这提供了有力的证据,我们应该将抗体视为完整的蛋白质,而不是功能区域的总和。

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