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DmpR 的 Y233 守门员调节 σ-RNA 聚合酶对效应子反应的转录控制。

The Y233 gatekeeper of DmpR modulates effector-responsive transcriptional control of σ -RNA polymerase.

机构信息

Department of Molecular Biology, Umeå University, SE-901 87, Umeå, Sweden.

Deparment of Chemistry, Umeå University, SE-901 87, Umeå, Sweden.

出版信息

Environ Microbiol. 2019 Apr;21(4):1321-1330. doi: 10.1111/1462-2920.14567. Epub 2019 Mar 7.

DOI:10.1111/1462-2920.14567
PMID:30773776
Abstract

DmpR is the obligate transcriptional activator of genes involved in (methyl)phenol catabolism by Pseudomonas putida. DmpR belongs to the AAA class of mechano-transcriptional regulators that employ ATP-hydrolysis to engage and remodel σ -RNA polymerase to allow transcriptional initiation. Previous work has established that binding of phenolic effectors by DmpR is a prerequisite to relieve interdomain repression and allow ATP-binding to trigger transition to its active multimeric conformation, and further that a structured interdomain linker between the effector- and ATP-binding domains is involved in coupling these processes. Here, we present evidence from ATPase and in vivo and in vitro transcription assays that a tyrosine residue of the interdomain linker (Y233) serves as a gatekeeper to constrain ATP-hydrolysis and aromatic effector-responsive transcriptional activation by DmpR. An alanine substitution of Y233A results in both increased ATPase activity and enhanced sensitivity to aromatic effectors. We propose a model in which effector-binding relocates Y233 to synchronize signal-reception with multimerisation to provide physiologically appropriate sensitivity of the transcriptional response. Given that Y233 counterparts are present in many ligand-responsive mechano-transcriptional regulators, the model is likely to be pertinent for numerous members of this family and has implications for development of enhanced sensitivity of biosensor used to detect pollutants.

摘要

DmpR 是 Pseudomonas putida 中(甲基)酚类物质代谢相关基因的必需转录激活因子。DmpR 属于 AAA 类机械转录调节因子,利用 ATP 水解来结合和重塑 σ-RNA 聚合酶,从而允许转录起始。先前的工作已经确定,DmpR 通过与酚类效应物的结合是解除结构域间抑制并允许 ATP 结合以触发其活性多聚体构象转变的前提条件,并且进一步的是,效应物结合和 ATP 结合结构域之间的结构域间连接体参与了这些过程的偶联。在这里,我们通过 ATP 酶以及体内和体外转录测定提供了证据,表明结构域间连接体中的一个酪氨酸残基(Y233)作为一个门卫,限制了 DmpR 的 ATP 水解和芳香族效应物响应的转录激活。用丙氨酸取代 Y233A 会导致 ATP 酶活性增加和对芳香族效应物的敏感性增强。我们提出了一个模型,其中效应物结合将 Y233 重新定位,以协调信号接收与多聚化,从而为转录反应提供生理上适当的敏感性。鉴于许多配体响应的机械转录调节因子都存在 Y233 对应物,该模型可能与该家族的许多成员有关,并对用于检测污染物的生物传感器的增强敏感性的发展具有重要意义。

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The Y233 gatekeeper of DmpR modulates effector-responsive transcriptional control of σ -RNA polymerase.DmpR 的 Y233 守门员调节 σ-RNA 聚合酶对效应子反应的转录控制。
Environ Microbiol. 2019 Apr;21(4):1321-1330. doi: 10.1111/1462-2920.14567. Epub 2019 Mar 7.
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引用本文的文献

1
Tetrameric architecture of an active phenol-bound form of the AAA transcriptional regulator DmpR.活性酚结合形式的 AAA 转录调节因子 DmpR 的四聚体结构。
Nat Commun. 2020 Jun 1;11(1):2728. doi: 10.1038/s41467-020-16562-5.