Engineering of the upper hinge region of human IgG1 Fc enhances the binding affinity to FcγIIIa (CD16a) receptor isoform.,Protein Engineering, Design and Selection

当前位置： X-MOL 学术 › Protein Eng. Des. Sel. › 论文详情

Our official English website, www.x-mol.net, welcomes your feedback! (Note: you will need to create a separate account there.)

Engineering of the upper hinge region of human IgG1 Fc enhances the binding affinity to FcγIIIa (CD16a) receptor isoform.
Protein Engineering, Design and Selection ( IF 2.6 ) Pub Date : 2018-10-10 , DOI: 10.1093/protein/gzy019
Dana N Ashoor ₁ , Noureddine Ben Khalaf ₁ , Sonia Bourguiba-Hachemi ₁ , Maryam H Marzouq ₁ , M Dahmani Fathallah ₁

Affiliation

The interaction between antibodies and Immune cells surface FcγRIIIa (CD16a) receptor triggers a variety of immune responses including antibody-dependent cell-mediated cytotoxicity, antibody neutralization, phagocytosis, inflammation and tissue injury. Recent studies showed that IgG1 upper hinge region and FcγRs polymorphism play a major role in the interaction with Fcγ receptors and in the stability of the immune complex hence, in mounting strong inflammatory response. To further investigate this issue, we developed a tool box of IgG1 Fc isoforms to depict the affinity between mutated IgG1 Fc regions and extracellular domain variants (V158F) of CD16a. Our strategy consisted of designing different random upper-hinge mutated variants of IgG1 Fc domain, reproducing the naturally occurring two variants of CD16a and producing all of them as recombinant fusion proteins in Pichia Pastoris. The interactions were assayed using the Surface Plasmon Resonance (Biacore) method along with an in silico analysis to identify the major interaction and key residues that underline the affinity between the Fc region and CD16a variants. Our data showed that the affinity of the Fc region to the CD16a is strongly correlated to polar interactions. This molecular engineering approach yielded an IgG1Fc mutant with enhanced binding affinity to CD16a F158 variant.

中文翻译：

人IgG1 Fc的上铰链区的工程设计增强了对FcγIIIa（CD16a）受体同工型的结合亲和力。

抗体与免疫细胞表面FcγRIIIa（CD16a）受体之间的相互作用触发各种免疫应答，包括抗体依赖性细胞介导的细胞毒性，抗体中和，吞噬作用，炎症和组织损伤。最近的研究表明，IgG1上铰链区和FcγRs多态性在与Fcγ受体的相互作用以及免疫复合物的稳定性中起着重要的作用，从而引起强烈的炎症反应。为了进一步研究这个问题，我们开发了一个IgG1 Fc亚型的工具箱来描述突变的IgG1 Fc区与CD16a的胞外域变体（V158F）之间的亲和力。我们的策略包括设计IgG1 Fc结构域的不同随机上铰链突变变体，克隆天然存在的两个CD16a变异体，并在巴斯德毕赤酵母中将它们全部制成重组融合蛋白。使用表面等离振子共振（Biacore）方法以及计算机分析来分析相互作用，从而鉴定出主要相互作用和关键残基，这些残基突出了Fc区与CD16a变体之间的亲和力。我们的数据表明，Fc区对CD16a的亲和力与极性相互作用密切相关。这种分子工程方法产生了对CD16a F158变体具有增强的结合亲和力的IgG1Fc突变体。使用表面等离振子共振（Biacore）方法以及计算机分析分析相互作用，以鉴定主要相互作用和关键残基，这些残基突出了Fc区与CD16a变体之间的亲和力。我们的数据表明，Fc区对CD16a的亲和力与极性相互作用密切相关。这种分子工程方法产生了对CD16a F158变体具有增强的结合亲和力的IgG1Fc突变体。使用表面等离振子共振（Biacore）方法以及计算机分析分析相互作用，以鉴定主要相互作用和关键残基，这些残基突出了Fc区与CD16a变体之间的亲和力。我们的数据表明，Fc区对CD16a的亲和力与极性相互作用密切相关。这种分子工程方法产生了对CD16a F158变体具有增强的结合亲和力的IgG1Fc突变体。

更新日期：2019-11-01

点击分享查看原文

点击收藏

公开下载

阅读更多本刊最新论文