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Examining weak protein-protein interactions in start codon recognition via nuclear magnetic resonance spectroscopy

机译:通过核磁共振波谱检查起始密码子识别中弱的蛋白质间相互作用

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摘要

Weak protein-protein interactions are critical in numerous biological processes. Unfortunately, they are difficult to characterize due to the high concentrations required for the production and detection of the complex population. The inherent sensitivity of nuclear magnetic resonance (NMR) spectroscopy to the chemical environment makes it an excellent tool to tackle this problem. NMR permits the exploration of interactions over a range of affinities, yielding essential insights into dynamic biological processes. The conversion of mRNA to protein is one such process that requires the coordinated association of many low affinity proteins. During start codon recognition, eukaryotic initiation factors assemble into high-order complexes that bind mRNA and bring it to the ribosome for decoding. Many of the structures of the eukaryotic initiation factors have been determined; however, only little is known regarding the weak binary complexes formed and their structure-function mechanisms. Herein, we use start codon recognition as a model system to review the relevant NMR methods for the characterization of weak interactions and the development of small molecule inhibitors.
机译:弱蛋白间相互作用在许多生物学过程中至关重要。不幸的是,由于生产和检测复杂种群所需的高浓度,它们难以表征。核磁共振(NMR)光谱对化学环境的固有敏感性使其成为解决此问题的绝佳工具。 NMR允许探索各种亲和力之间的相互作用,从而获得对动态生物学过程的基本见解。从mRNA到蛋白质的转化就是这样一种过程,它需要许多低亲和力蛋白的协调结合。在起始密码子识别过程中,真核生物起始因子组装成高阶复合物,这些复合物结合mRNA,并将其带入核糖体进行解码。真核生物起始因子的许多结构已经确定。然而,关于形成的弱二元络合物及其结构-作用机理知之甚少。在本文中,我们使用起始密码子识别作为模型系统来审查相关的NMR方法,以表征弱相互作用和开发小分子抑制剂。

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