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探讨沙眼衣原体 III 型分泌伴侣复合物 Scc4:Scc1 在大肠杆菌中的顺序表达的关联。

Insights into the association of the Chlamydia trachomatis type III secretion chaperone complex, Scc4:Scc1, from sequential expression in Escherichia coli.

机构信息

Department of Chemistry, Louisiana State University, Baton Rouge, LA, 70803, United States.

Department of Microbiology, Immunology, and Parasitology, Louisiana State University Health Sciences Center, New Orleans, LA, 70112, United States.

出版信息

Protein Expr Purif. 2024 Oct;222:106532. doi: 10.1016/j.pep.2024.106532. Epub 2024 Jun 8.

DOI:10.1016/j.pep.2024.106532
PMID:38857716
Abstract

Chlamydia trachomatis (CT) is the bacterial pathogen responsible for causing the most common sexually transmitted disease in the United States. This obligate, intracellular Gram-negative bacterium has a type III secretion system (T3SS) to invade host cells. CopN is an important effector, plug protein that mediates early interactions between the host and Chlamydia. CopN is chaperoned by a heterodimer, T3SS chaperone complex containing Scc4 and Scc1. Scc4 is a unique, bifunctional protein that, in addition to its T3SS chaperone activity, acts as an RNA polymerase (RNAP) binding protein. We hypothesized that the two functions occur at different points in CT's developmental cycle with Scc4 acting alone in the early-to-mid stages and the Scc4:Scc1 complex chaperoning CopN in the mid-to-late stages. To study the Scc4:Scc1 complex by NMR, we previously explored various methods of associating Scc4 and Scc1 in vitro to produce the complex with chain-selective isotopic labeling. Though co-expressed Scc4 and Scc1 form a stable complex, the in vitro association studies suggest that partial protein denaturation and/or components in E. coli lysate are necessary to form the stable complex. In this study Scc4 and Scc1 were sequentially expressed in E. coli under the control of different promoters, allowing separate isotopic labeling of each chain and complex formation in vivo. Sequential expression resulted in no or unstable complex formation depending on the culture medium used. These results, taken together with previous in vitro association studies, suggest that Scc4 and Scc1 assemble co-translationally to form the stable Scc4:Scc1 complex in E. coli.

摘要

沙眼衣原体(CT)是导致美国最常见性传播疾病的细菌病原体。这种专性、细胞内革兰氏阴性菌具有 III 型分泌系统(T3SS)以入侵宿主细胞。CopN 是一种重要的效应子、塞子蛋白,介导宿主与衣原体之间的早期相互作用。CopN 由 T3SS 伴侣复合物(包含 Scc4 和 Scc1)的异二聚体伴侣。Scc4 是一种独特的双功能蛋白,除了其 T3SS 伴侣活性外,还作为 RNA 聚合酶(RNAP)结合蛋白。我们假设这两个功能发生在 CT 的发育周期的不同点,Scc4 在早期到中期单独作用,而 Scc4:Scc1 复合物在中期到晚期伴侣 CopN。为了通过 NMR 研究 Scc4:Scc1 复合物,我们之前探索了各种体外关联 Scc4 和 Scc1 的方法,以产生具有链选择性同位素标记的复合物。尽管共表达的 Scc4 和 Scc1 形成稳定的复合物,但体外关联研究表明,部分蛋白质变性和/或大肠杆菌裂解物中的成分是形成稳定复合物所必需的。在这项研究中,Scc4 和 Scc1 在大肠杆菌中分别在不同启动子的控制下表达,允许每个链的单独同位素标记和体内复合物形成。根据使用的培养基,序列表达导致没有或不稳定的复合物形成。这些结果与之前的体外关联研究一起表明,Scc4 和 Scc1 以共翻译的方式组装形成大肠杆菌中稳定的 Scc4:Scc1 复合物。

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