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核糖体蛋白网络在核糖体动力学中的作用。

The role of ribosomal protein networks in ribosome dynamics.

作者信息

Timsit Youri, Sergeant-Perthuis Grégoire, Bennequin Daniel

机构信息

Aix Marseille Univ, Université de Toulon, CNRS, IRD, MIO UM110, 163 avenue de Luminy 13288 Marseille, France.

Research Federation for the Study of Global Ocean Systems Ecology and Evolution, FR2022/Tara GOSEE, 3 Rue Michel-Ange, 75016 Paris, France.

出版信息

Nucleic Acids Res. 2025 Jan 7;53(1). doi: 10.1093/nar/gkae1308.

Abstract

Accurate protein synthesis requires ribosomes to integrate signals from distant functional sites and execute complex dynamics. Despite advances in understanding ribosome structure and function, two key questions remain: how information is transmitted between these distant sites, and how ribosomal movements are synchronized? We recently highlighted the existence of ribosomal protein networks, likely evolved to participate in ribosome signaling. Here, we investigate the relationship between ribosomal protein networks and ribosome dynamics. Our findings show that major motion centers in the bacterial ribosome interact specifically with r-proteins, and that ribosomal RNA exhibits high mobility around each r-protein. This suggests that periodic electrostatic changes in the context of negatively charged residues (Glu and Asp) induce RNA-protein 'distance-approach' cycles, controlling key ribosomal movements during translocation. These charged residues play a critical role in modulating electrostatic repulsion between RNA and proteins, thus coordinating ribosomal dynamics. We propose that r-protein networks synchronize ribosomal dynamics through an 'electrostatic domino' effect, extending the concept of allostery to the regulation of movements within supramolecular assemblies.

摘要

准确的蛋白质合成需要核糖体整合来自远处功能位点的信号并执行复杂的动力学过程。尽管在理解核糖体结构和功能方面取得了进展,但仍存在两个关键问题:信息如何在这些远处位点之间传递,以及核糖体运动如何同步?我们最近强调了核糖体蛋白网络的存在,其可能进化而来参与核糖体信号传导。在此,我们研究核糖体蛋白网络与核糖体动力学之间的关系。我们的研究结果表明,细菌核糖体中的主要运动中心与核糖体蛋白特异性相互作用,并且核糖体RNA在每个核糖体蛋白周围表现出高流动性。这表明在带负电荷的残基(谷氨酸和天冬氨酸)环境中的周期性静电变化会诱导RNA - 蛋白质的“距离 - 接近”循环,从而在转位过程中控制关键的核糖体运动。这些带电荷的残基在调节RNA和蛋白质之间的静电排斥中起关键作用,从而协调核糖体动力学。我们提出核糖体蛋白网络通过“静电多米诺骨牌”效应使核糖体动力学同步,将变构概念扩展到超分子组装体内运动的调节。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/594b/11711686/001ace80ede1/gkae1308figgra1.jpg

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