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预测无序蛋白质的构象集合:从分子动力学到机器学习。

Predicting Conformational Ensembles of Intrinsically Disordered Proteins: From Molecular Dynamics to Machine Learning.

机构信息

CNR-IOM at International School for Advanced Studies (SISSA/ISAS), via Bonomea 265, 34136 Trieste, Italy.

Department of Chemistry, Faculty of Exact Sciences and the Institute for Nanotechnology and Advanced Materials (BINA), Bar-Ilan University, 5290002 Ramat-Gan, Israel.

出版信息

J Phys Chem Lett. 2024 Aug 15;15(32):8177-8186. doi: 10.1021/acs.jpclett.4c01544. Epub 2024 Aug 2.

Abstract

Intrinsically disordered proteins and regions (IDP/IDRs) are ubiquitous across all domains of life. Characterized by a lack of a stable tertiary structure, IDP/IDRs populate a diverse set of transiently formed structural states that can promiscuously adapt upon binding with specific interaction partners and/or certain alterations in environmental conditions. This malleability is foundational for their role as tunable interaction hubs in core cellular processes such as signaling, transcription, and translation. Tracing the conformational ensemble of an IDP/IDR and its perturbation in response to regulatory cues is thus paramount for illuminating its function. However, the conformational heterogeneity of IDP/IDRs poses several challenges. Here, we review experimental and computational methods devised to disentangle the conformational landscape of IDP/IDRs, highlighting recent computational advances that permit proteome-wide scans of IDP/IDRs conformations. We briefly evaluate selected computational methods using the disordered N-terminal of the human copper transporter 1 as a test case and outline further challenges in IDP/IDRs ensemble prediction.

摘要

无规卷曲蛋白质和区域 (IDP/IDRs) 在所有生命领域中普遍存在。IDP/IDRs 的特征是缺乏稳定的三级结构,它们存在于一系列多样化的瞬态形成的结构状态中,可以在与特定相互作用伙伴结合时以及/或者在环境条件发生某些改变时随意适应。这种可塑性是它们作为核心细胞过程(如信号转导、转录和翻译)中可调相互作用中心的基础。因此,追踪 IDP/IDR 的构象整体及其对调节信号的扰动对于阐明其功能至关重要。然而,IDP/IDRs 的构象异质性带来了一些挑战。在这里,我们综述了用于解析 IDP/IDRs 构象景观的实验和计算方法,重点介绍了最近允许对 IDP/IDRs 构象进行全蛋白质组扫描的计算进展。我们使用人类铜转运蛋白 1 的无规卷曲 N 端作为测试案例简要评估了选定的计算方法,并概述了 IDP/IDRs 整体预测中的进一步挑战。

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