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OpaR 通过其对 ScrC 的调节和触发磷酸二酯酶 TpdA 对 c-di-GMP 动态平衡和在 中的表达进行了动态控制。

OpaR Exerts a Dynamic Control over c-di-GMP Homeostasis and Expression in through Its Regulation of ScrC and the Trigger Phosphodiesterase TpdA.

机构信息

Programa de Microbiología Genómica, Centro de Ciencias Genómicas, Universidad Nacional Autónoma de México, Cuernavaca, Morelos, Mexico.

出版信息

Microbiol Spectr. 2023 Jun 15;11(3):e0087223. doi: 10.1128/spectrum.00872-23. Epub 2023 May 18.

Abstract

The second messenger cyclic dimeric GMP (c-di-GMP) plays a central role in controlling decision-making processes that are vitally important for the environmental survival of the human pathogen Vibrio parahaemolyticus. The mechanisms by which c-di-GMP levels and biofilm formation are dynamically controlled in V. parahaemolyticus are poorly understood. Here, we report the involvement of OpaR in controlling c-di-GMP metabolism and its effects on the expression of the trigger phosphodiesterase (PDE) TpdA and the biofilm-matrix related gene . Our results revealed that OpaR negatively modulates the expression of by maintaining a baseline level of c-di-GMP. The OpaR-regulated PDEs ScrC, ScrG, and VP0117 enable the upregulation of , to different degrees, in the absence of OpaR. We also found that TpdA plays the dominant role in c-di-GMP degradation under planktonic conditions compared to the other OpaR-regulated PDEs. In cells growing on solid medium, we observed that the role of the dominant c-di-GMP degrader alternates between ScrC and TpdA. We also report contrasting effects of the absence of OpaR on expression in cells growing on solid media compared to cells forming biofilms over glass. These results suggest that OpaR can act as a double-edged sword to control expression and perhaps biofilm development in response to poorly understood environmental factors. Finally, using an analysis, we indicate outlets of the OpaR regulatory module that can impact decision making during the motile-to-sessile transition in V. parahaemolyticus. The second messenger c-di-GMP is extensively used by bacterial cells to control crucial social adaptations such as biofilm formation. Here, we explore the role of the quorum-sensing regulator OpaR, from the human pathogen V. parahaemolyticus, on the dynamic control of c-di-GMP signaling and biofilm-matrix production. We found that OpaR is crucial to c-di-GMP homeostasis in cells growing on Lysogeny Broth agar and that the OpaR-regulated PDEs TpdA and ScrC alternate in the dominant role over time. Furthermore, OpaR plays contrasting roles in controlling the expression of the biofilm-related gene on different surfaces and growth conditions. This dual role has not been reported for orthologues of OpaR, such as HapR from Vibrio cholerae. It is important to investigate the origins and consequences of the differences in c-di-GMP signaling between closely and distantly related pathogens to better understand pathogenic bacterial behavior and its evolution.

摘要

第二信使环二鸟苷酸 (c-di-GMP) 在控制人类病原体副溶血性弧菌的环境生存至关重要的决策过程中发挥着核心作用。c-di-GMP 水平和生物膜形成的动态控制机制在副溶血性弧菌中还知之甚少。在这里,我们报告了 OpaR 参与控制 c-di-GMP 代谢及其对触发磷酸二酯酶 (PDE) TpdA 和生物膜基质相关基因 的表达的影响。我们的结果表明,OpaR 通过维持 c-di-GMP 的基线水平来负调控 的表达。OpaR 调节的 PDEs ScrC、ScrG 和 VP0117 能够在没有 OpaR 的情况下不同程度地上调 。我们还发现,与其他 OpaR 调节的 PDE 相比,TpdA 在浮游状态下的 c-di-GMP 降解中起主导作用。在固体培养基上生长的细胞中,我们观察到主导 c-di-GMP 降解酶 ScrC 和 TpdA 之间的作用在不断交替。我们还报告了与生物膜相比,OpaR 缺失对固体培养基上细胞 表达的影响与玻璃上形成生物膜的细胞不同。这些结果表明,OpaR 可以作为一把双刃剑,根据未知的环境因素控制 的表达和生物膜的发育。最后,我们使用 RNA-seq 分析指出了 OpaR 调节模块的出口,这些出口可能会影响副溶血性弧菌从游动到静止状态的过渡中的决策。第二信使 c-di-GMP 被细菌细胞广泛用于控制生物膜形成等关键的社会适应。在这里,我们探索了人类病原体副溶血性弧菌的群体感应调节剂 OpaR 在动态控制 c-di-GMP 信号和生物膜基质产生中的作用。我们发现,OpaR 对在 Lysogeny Broth 琼脂上生长的细胞中的 c-di-GMP 动态平衡至关重要,并且 OpaR 调节的 PDEs TpdA 和 ScrC 随着时间的推移会交替发挥主导作用。此外,OpaR 在控制生物膜相关基因 在不同表面和生长条件下的表达方面发挥着相反的作用。这种双重作用尚未在 OpaR 的同源物(如霍乱弧菌的 HapR)中报道过。研究密切和远距离相关病原体之间 c-di-GMP 信号的差异的起源和后果对于更好地理解致病菌的行为及其进化非常重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/25c8/10269520/ed9dee19374e/spectrum.00872-23-f001.jpg

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