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通过不同蛋白质亚结构的模块化替换研究细菌信号转导蛋白ToxR的膜插入及转录激活需求。

Membrane insertion of the bacterial signal transduction protein ToxR and requirements of transcription activation studied by modular replacement of different protein substructures.

作者信息

Kolmar H, Hennecke F, Götze K, Janzer B, Vogt B, Mayer F, Fritz H J

机构信息

Institut für Molekulare Genetik, George-August-Universität Göttingen, Germany.

出版信息

EMBO J. 1995 Aug 15;14(16):3895-904. doi: 10.1002/j.1460-2075.1995.tb00061.x.

Abstract

The Vibrio cholerae protein ToxR is an integral membrane protein that acts as a transcription activator in response to environmental signals; it controls expression of toxin genes ctxA and ctxB, along with a variety of other genes related to pathogenicity. Here it is shown that: (i) ToxR has a modular architecture and that activation of transcription starting at the ctx promoter depends strictly on dimerization of the periplasmic ToxR domain; (ii) the transmembrane (TM) region of ToxR is sufficient as a topogenic signal but not for stable membrane anchoring of the protein; (iii) the TM region has no special function in signal transduction and (iv) a proline residue located within the TM region minimizes background transcription activation, most plausibly by reducing TM-TM interaction. Possible applications of ToxR as a technical tool for analysing protein-protein interactions between pairs of arbitrary TM domains are discussed.

摘要

霍乱弧菌蛋白ToxR是一种整合膜蛋白,可作为响应环境信号的转录激活因子;它控制毒素基因ctxA和ctxB的表达,以及与致病性相关的多种其他基因的表达。本文表明:(i)ToxR具有模块化结构,并且从ctx启动子开始的转录激活严格依赖于周质ToxR结构域的二聚化;(ii)ToxR的跨膜(TM)区域足以作为拓扑信号,但不足以实现该蛋白的稳定膜锚定;(iii)TM区域在信号转导中没有特殊功能;(iv)位于TM区域内的一个脯氨酸残基最有可能通过减少TM-TM相互作用来最小化背景转录激活。本文还讨论了ToxR作为分析任意一对TM结构域之间蛋白质-蛋白质相互作用的技术工具的可能应用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/45b0/394468/89dad5bae63d/emboj00040-0054-a.jpg

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