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Ensembles in solution as a new paradigm for antibody structure prediction and design

机译:在解决方案中作为抗体结构预测和设计的新范式组合

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摘要

The rise of antibodies as a promising and rapidly growing class of biotherapeutic proteins has motivated numerous studies to characterize and understand antibody structures. In the past decades, the number of antibody crystal structures increased substantially, which revolutionized the atomistic understanding of antibody functions. Even though numerous static structures are known, various biophysical properties of antibodies (i.e., specificity, hydrophobicity and stability) are governed by their dynamic character. Additionally, the importance of high-quality structures in structure–function relationship studies has substantially increased. These structure–function relationship studies have also created a demand for precise homology models of antibody structures, which allow rational antibody design and engineering when no crystal structure is available. Here, we discuss various aspects and challenges in antibody design and extend the paradigm of describing antibodies with only a single static structure to characterizing them as dynamic ensembles in solution.
机译:抗体作为有前途和快速增长的生物治疗蛋白的兴起具有许多研究表征和理解抗体结构的研究。在过去几十年中,抗体晶体结构的数量大幅增加,这促进了对抗体功能的原子理解。尽管已知许多静态结构,但抗体的各种生物物理性质(即特异性,疏水性和稳定性)是由其动态特征的控制。另外,高质量结构在结构功能关系研究中的重要性大大增加。这些结构功能关系研究还创造了对抗体结构的精确同源性模型的需求,这允许在没有晶体结构时允许合理的抗体设计和工程。在这里,我们讨论抗体设计中的各个方面和挑战,并扩展了描述抗体的范例,只有单个静态结构,以表征它们在溶液中的动态集合。

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