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穿越细菌边界:恶臭假单胞菌 KT2440 的碳分解代谢物阻遏系统 Crc-Hfq 作为控制大肠杆菌翻译的工具。

Crossing bacterial boundaries: The carbon catabolite repression system Crc-Hfq of Pseudomonas putida KT2440 as a tool to control translation in E. coli.

机构信息

Bioprocess Engineering, Wageningen University and Research, 6700AA Wageningen, The Netherlands.

Bioprocess Engineering, Wageningen University and Research, 6700AA Wageningen, The Netherlands.

出版信息

N Biotechnol. 2023 Nov 25;77:20-29. doi: 10.1016/j.nbt.2023.06.004. Epub 2023 Jun 20.

DOI:10.1016/j.nbt.2023.06.004
PMID:37348756
Abstract

As a global regulatory mechanism, carbon catabolite repression allows bacteria and eukaryal microbes to preferentially utilize certain substrates from a mixture of carbon sources. The mechanism varies among different species. In Pseudomonas spp., it is mainly mediated by the Crc-Hfq complex which binds to the 5' region of the target mRNAs, thereby inhibiting their translation. This molecular mechanism enables P. putida to rapidly adjust and fine-tune gene expression in changing environments. Hfq is an RNA-binding protein that is ubiquitous and highly conserved in bacterial species. Considering the characteristics of Hfq, and the widespread use and rapid response of Crc-Hfq in P. putida, this complex has the potential to become a general toolbox for post-transcriptional multiplex regulation. In this study, we demonstrate for the first time that transplanting the pseudomonal catabolite repression protein, Crc, into E. coli causes multiplex gene repression. Under the control of Crc, the production of a diester and its precursors was significantly reduced. The effects of Crc introduction on cell growth in both minimal and rich media were evaluated. Two potential factors - off-target effects and Hfq-sequestration - could explain negative effects on cell growth. Simultaneous reduction of off-targeting and increased sequestration of Hfq by the introduction of the small RNA CrcZ, indicated that Hfq sequestration plays a more prominent role in the negative side-effects. This suggests that the negative growth effect can be mitigated by well-controlled expression of Hfq. This study reveals the feasibility of controlling gene expression using heterologous regulation systems.

摘要

作为一种全球调控机制,碳分解代谢物阻遏允许细菌和真核微生物优先利用混合物中的某些碳源。其机制在不同物种之间有所不同。在假单胞菌属中,它主要由 Crc-Hfq 复合物介导,该复合物结合到靶 mRNA 的 5'区域,从而抑制其翻译。这种分子机制使 P. putida 能够在不断变化的环境中快速调整和微调基因表达。Hfq 是一种 RNA 结合蛋白,在细菌物种中普遍存在且高度保守。考虑到 Hfq 的特点以及 Crc-Hfq 在 P. putida 中的广泛应用和快速响应,该复合物有可能成为转录后多重调控的通用工具箱。在这项研究中,我们首次证明将假单胞菌分解代谢物阻遏蛋白 Crc 移植到大肠杆菌中会导致多重基因抑制。在 Crc 的控制下,二酯及其前体的产量明显降低。评估了 Crc 引入对最小和丰富培养基中细胞生长的影响。两种潜在因素——脱靶效应和 Hfq 隔离——可以解释对细胞生长的负面影响。通过引入小 RNA CrcZ 同时减少脱靶和增加 Hfq 的隔离,表明 Hfq 隔离在负面副作用中起着更突出的作用。这表明通过 Hfq 的受控表达可以减轻负生长效应。这项研究揭示了使用异源调控系统控制基因表达的可行性。

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