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对EccD进行深度突变扫描揭示了其在分枝杆菌ESX分泌系统中不可或缺性的分子基础。

Deep mutational scanning of EccD reveals the molecular basis of its essentiality in the mycobacterium ESX secretion system.

作者信息

Trinidad Donovan D, Macdonald Christian B, Rosenberg Oren S, Fraser James S, Coyote-Maestas Willow

机构信息

Department of Medicine, University of California, San Francisco.

Department of Bioengineering and Therapeutic Sciences, University of California, San Francisco, San Francisco, CA 94158, USA.

出版信息

bioRxiv. 2024 Aug 24:2024.08.23.609456. doi: 10.1101/2024.08.23.609456.

Abstract

Tuberculosis remains the deadliest infectious disease in the world and requires novel therapeutic targets. The ESX-3 secretion system, which is essential for iron and zinc homeostasis and thus survival, is a promising target. In this study, we perform a deep mutational scan on the ESX-3 core protein EccD in the model organism . We systematically investigated the functional roles of 145 residues across the soluble ubiquitin-like domain, the conformationally distinct flexible linker, and selected transmembrane helices of EccD. Our data combined with structural comparisons to ESX-5 complexes support a model where EccD stabilizes the complex, with the hinge motif within the linker being particularly sensitive to disruption. Our study is the first deep mutational scan in mycobacteria, which could help guide drug development toward novel treatment of tuberculosis. This study underscores the importance of context-specific mutational analyses for discovering essential protein interactions within mycobacterial systems.

摘要

结核病仍然是世界上最致命的传染病,需要新的治疗靶点。ESX-3分泌系统对铁和锌的稳态以及生存至关重要,是一个有前景的靶点。在本研究中,我们在模式生物中对ESX-3核心蛋白EccD进行了深度突变扫描。我们系统地研究了EccD的可溶性泛素样结构域、构象不同的柔性连接子以及选定的跨膜螺旋上145个残基的功能作用。我们的数据与ESX-5复合物的结构比较相结合,支持了一个模型,即EccD稳定复合物,连接子内的铰链基序对破坏特别敏感。我们的研究是分枝杆菌中的首次深度突变扫描,有助于指导针对结核病新疗法的药物开发。这项研究强调了针对特定背景的突变分析对于发现分枝杆菌系统内必需蛋白质相互作用的重要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/afd8/11370616/a44b25fff473/nihpp-2024.08.23.609456v1-f0001.jpg

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