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一种基于受体的开关,调节炭疽毒素孔形成。

A receptor-based switch that regulates anthrax toxin pore formation.

机构信息

Nomis Center for Immunobiology and Microbial Pathogenesis, The Salk Institute for Biological Studies, La Jolla, California, United States of America.

出版信息

PLoS Pathog. 2011 Dec;7(12):e1002354. doi: 10.1371/journal.ppat.1002354. Epub 2011 Dec 8.

Abstract

Cellular receptors can act as molecular switches, regulating the sensitivity of microbial proteins to conformational changes that promote cellular entry. The activities of these receptor-based switches are only partially understood. In this paper, we sought to understand the mechanism that underlies the activity of the ANTXR2 anthrax toxin receptor-based switch that binds to domains 2 and 4 of the protective antigen (PA) toxin subunit. Receptor-binding restricts structural changes within the heptameric PA prepore that are required for pore conversion to an acidic endosomal compartment. The transfer cross-saturation (TCS) NMR approach was used to monitor changes in the heptameric PA-receptor contacts at different steps during prepore-to-pore conversion. These studies demonstrated that receptor contact with PA domain 2 is weakened prior to pore conversion, defining a novel intermediate in this pathway. Importantly, ANTXR2 remained bound to PA domain 4 following pore conversion, suggesting that the bound receptor might influence the structure and/or function of the newly formed pore. These studies provide new insights into the function of a receptor-based molecular switch that controls anthrax toxin entry into cells.

摘要

细胞受体可以作为分子开关,调节微生物蛋白对构象变化的敏感性,促进细胞进入。这些基于受体的开关的活性仅部分被理解。在本文中,我们试图了解基于 ANTXR2 炭疽毒素受体的开关的活性机制,该开关结合保护性抗原 (PA) 毒素亚基的结构域 2 和 4。受体结合限制了七聚体 PA 前孔内对于孔转化为酸性内体隔室所必需的结构变化。转移交叉饱和 (TCS) NMR 方法用于监测在预孔到孔转化过程中的不同步骤中七聚体 PA-受体接触的变化。这些研究表明,在孔转化之前,PA 结构域 2 与受体的接触减弱,定义了该途径中的一个新的中间产物。重要的是,ANTXR2 在孔转化后仍与 PA 结构域 4 结合,这表明结合的受体可能影响新形成的孔的结构和/或功能。这些研究为控制炭疽毒素进入细胞的基于受体的分子开关的功能提供了新的见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7e79/3234216/968d2ef4f3a1/ppat.1002354.g001.jpg

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