Bispecific antibodies-effects of point mutations on CH3-CH3 interface stability.

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS

ACS Applied Bio Materials Pub Date : 2022-02-17 DOI:10.1093/protein/gzac012

Nancy D Pomarici, Monica L Fernández-Quintero, Patrick K Quoika, Franz Waibl, Alexander Bujotzek, Guy Georges, Klaus R Liedl

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Abstract

A new format of therapeutic proteins is bispecific antibodies, in which two different heavy chains heterodimerize to obtain two different binding sites. Therefore, it is crucial to understand and optimize the third constant domain (CH3-CH3) interface to favor heterodimerization over homodimerization, and to preserve the physicochemical properties, as thermal stability. Here, we use molecular dynamics simulations to investigate the dissociation process of 19 CH3-CH3 crystal structures that differ from each other in few point mutations. We describe the dissociation of the dimeric interface as a two-steps mechanism. As confirmed by a Markov state model, apart from the bound and the dissociated state, we observe an additional intermediate state, which corresponds to an encounter complex. The analysis of the interdomain contacts reveals key residues that stabilize the interface. We expect that our results will improve the understanding of the CH3-CH3 interface interactions and thus advance the developability and design of new antibodies formats.

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点突变对 CH3-CH3 界面稳定性的影响。

双特异性抗体是治疗蛋白的一种新形式，其中两条不同的重链通过异源二聚化获得两个不同的结合位点。因此，了解并优化第三恒定结构域（CH3-CH3）界面，使其有利于异源二聚化而不是同源二聚化，并保持其热稳定性等理化特性至关重要。在这里，我们利用分子动力学模拟研究了 19 个 CH3-CH3 晶体结构的解离过程，这些晶体结构因几个点突变而彼此不同。我们将二聚体界面的解离过程描述为两步机制。正如马尔可夫状态模型所证实的那样，除了结合态和解离态之外，我们还观察到一个额外的中间状态，它对应于一个相遇复合物。对域间接触的分析揭示了稳定界面的关键残基。我们希望我们的研究结果能加深人们对 CH3-CH3 界面相互作用的理解，从而推动新抗体形式的开发和设计。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

ACS Applied Bio Materials Chemistry-Chemistry (all)

CiteScore

9.40

自引率

2.10%

发文量

464