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pH 触发的构象转换沿着白喉毒素 T 结构域的膜插入途径。

pH-triggered conformational switching along the membrane insertion pathway of the diphtheria toxin T-domain.

机构信息

Department of Biochemistry and Molecular Biology, The University of Kansas Medical Center, Kansas City, KS 66160, USA.

出版信息

Toxins (Basel). 2013 Aug 6;5(8):1362-80. doi: 10.3390/toxins5081362.

Abstract

The translocation (T)-domain plays a key role in the action of diphtheria toxin and is responsible for transferring the catalytic domain across the endosomal membrane into the cytosol in response to acidification. Deciphering the molecular mechanism of pH-dependent refolding and membrane insertion of the T-domain, which is considered to be a paradigm for cell entry of other bacterial toxins, reveals general physicochemical principles underlying membrane protein assembly and signaling on membrane interfaces. Structure-function studies along the T-domain insertion pathway have been affected by the presence of multiple conformations at the same time, which hinders the application of high-resolution structural techniques. Here, we review recent progress in structural, functional and thermodynamic studies of the T-domain archived using a combination of site-selective fluorescence labeling with an array of spectroscopic techniques and computer simulations. We also discuss the principles of conformational switching along the insertion pathway revealed by studies of a series of T-domain mutants with substitutions of histidine residues.

摘要

易位(T)结构域在白喉毒素的作用中起着关键作用,负责在酸性条件下将催化结构域从内体膜转移到细胞质中。解析 T 结构域 pH 依赖性重折叠和膜插入的分子机制,这被认为是其他细菌毒素进入细胞的范例,揭示了膜蛋白组装和膜界面信号传递的一般物理化学原理。结构-功能研究沿着 T 结构域插入途径受到同时存在多种构象的影响,这阻碍了高分辨率结构技术的应用。在这里,我们综述了使用一系列光谱技术和计算机模拟与位点选择性荧光标记相结合的方法,对 T 结构域进行结构、功能和热力学研究的最新进展。我们还讨论了通过一系列 T 结构域突变体的取代研究揭示的插入途径中构象转换的原理。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/48e6/3760040/a3a0451f25e4/toxins-05-01362-g001.jpg

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