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营养物质对衣原体Rsb伴侣切换机制功能的影响。

Impact of nutrients on the function of the chlamydial Rsb partner switching mechanism.

作者信息

Kuwabara Shiomi, Landers Evan R, Fisher Derek J

机构信息

Molecular Biology, Microbiology and Biochemistry Graduate Program, Southern Illinois University, Carbondale, IL 62901, United States.

School of Biological Sciences, Southern Illinois University, Carbondale, IL 62901, United States.

出版信息

Pathog Dis. 2022 Nov 29;80(1). doi: 10.1093/femspd/ftac044.

Abstract

The obligate intracellular bacterial pathogen Chlamydia trachomatis is a leading cause of sexually transmitted infections and infectious blindness. Chlamydia undergo a biphasic developmental cycle alternating between the infectious elementary body (EB) and the replicative reticulate body (RB). The molecular mechanisms governing RB growth and RB-EB differentiation are unclear. We hypothesize that the bacterium senses host cell and bacterial energy levels and metabolites to ensure that development and growth coincide with nutrient availability. We predict that a partner switching mechanism (PSM) plays a key role in the sensing and response process acting as a molecular throttle sensitive to metabolite levels. Using purified wild type and mutant PSM proteins, we discovered that metal type impacts enzyme activity and the substrate specificity of RsbU and that RsbW prefers ATP over GTP as a phosphate donor. Immunoblotting analysis of RsbV1/V2 demonstrated the presence of both proteins beyond 20 hours post infection and we observed that an RsbV1-null strain has a developmental delay and exhibits differential growth attenuation in response to glucose levels. Collectively, our data support that the PSM regulates growth in response to metabolites and further defines biochemical features governing PSM-component interactions which could help in the development of novel PSM-targeted therapeutics.

摘要

专性胞内细菌病原体沙眼衣原体是性传播感染和感染性失明的主要原因。衣原体经历双相发育周期,在感染性原体(EB)和复制性网状体(RB)之间交替。控制RB生长和RB-EB分化的分子机制尚不清楚。我们假设该细菌感知宿主细胞和细菌的能量水平及代谢物,以确保发育和生长与营养物质的可利用性相一致。我们预测一种伴侣切换机制(PSM)在传感和反应过程中起关键作用,作为对代谢物水平敏感的分子节流器。使用纯化的野生型和突变型PSM蛋白,我们发现金属类型会影响RsbU的酶活性和底物特异性,并且RsbW更倾向于ATP而非GTP作为磷酸供体。对RsbV1/V2的免疫印迹分析表明,在感染后20小时以上这两种蛋白均存在,并且我们观察到RsbV1缺失菌株存在发育延迟,并对葡萄糖水平表现出不同的生长衰减。总体而言,我们的数据支持PSM响应代谢物调节生长,并进一步定义了控制PSM组分相互作用的生化特征,这可能有助于开发新型的靶向PSM的疗法。

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