蛋白质动力学
动力学(音乐)
分子动力学
解码方法
计算机科学
生物系统
内在无序蛋白质
计算生物学
杠杆(统计)
化学
生物物理学
生物
算法
物理
人工智能
计算化学
声学
作者
Beirong Zhang,Zhou Gong,Lili Zhao,Yuxin An,Hang Gao,Jing Chen,Zhen Liang,Maili Liu,Yukui Zhang,Qun Zhao,Lihua Zhang
标识
DOI:10.1002/anie.202301345
摘要
Protein dynamics play a crucial role in their diverse functions. The intracellular environment significantly influences protein dynamics, particularly for intrinsically disordered proteins (IDPs). To comprehensively capture structural information from various proteins within cells and characterize protein dynamics, chemical cross-linking mass spectrometry was employed. In this study, we introduce a hierarchical decoding strategy that enables the investigation of protein dynamics in vivo. Computational analysis based on distance restraints derived from cross-links is used to infer protein dynamics in cells. To facilitate this analysis, we leverage the prior structure obtained from AlphaFold2. By employing this strategy, we can characterize the full-length structure of multi-domain proteins taking into account their distinct dynamic features. Furthermore, by combining restraint sampling with an unbiased sampling and evaluation approach, we can provide a comprehensive description of the intrinsic motion of IDPs. Consequently, the hierarchical strategy we propose holds significant potential in advancing our understanding of the molecular mechanisms that undelie protein functions in cells.
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