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环二鸟苷酸调控 CckA-ChpT-CtrA 磷酸传递系统双向控制荚膜红细菌基因转导颗粒的产生

The CckA-ChpT-CtrA Phosphorelay Controlling Rhodobacter capsulatus Gene Transfer Agent Production Is Bidirectional and Regulated by Cyclic di-GMP.

机构信息

Department of Microbiology and Immunology, University of British Columbia, Vancouver, British Columbia, Canada.

Department of Biology, Memorial University of Newfoundland, St. John's, Newfoundland and Labrador, Canada.

出版信息

J Bacteriol. 2021 Feb 8;203(5). doi: 10.1128/JB.00525-20.

Abstract

Protein phosphorylation is a universal mechanism for transducing cellular signals in prokaryotes and eukaryotes. The histidine kinase CckA, the histidine phosphotransferase ChpT, and the response regulator CtrA are conserved throughout the alphaproteobacteria. In , these proteins are key regulators of the gene transfer agent (RcGTA), which is present in several alphaproteobacteria. Using purified recombinant proteins, we show autophosphorylation of CckA protein, and phosphotransfer to ChpT and thence to CtrA, to demonstrate biochemically that they form a phosphorelay. The secondary messenger cyclic di-GMP changed CckA from a kinase to a phosphatase, resulting in reversal of the phosphotransfer flow in the relay. The substitutions of two residues in CckA greatly affected the kinase or phosphatase activity of the protein , and production of mutant CckA proteins confirmed the importance of kinase but not phosphatase activity for the lytic release of RcGTA. However, phosphatase activity was needed to produce functional RcGTA particles. The binding of cyclic di-GMP to the wild-type and mutant CckA proteins was evaluated directly using a pulldown assay based on biotinylated cyclic di-GMP and streptavidin-linked beads. The CckA, ChpT, and CtrA phosphorelay proteins are widespread in the alphaproteobacteria, and there are two groups of organisms that differ in terms of whether this pathway is essential for cell viability. Little is known about the biochemical function of these proteins in organisms where the pathway is not essential, a group that includes This work demonstrates biochemically that CckA, ChpT, and CtrA also form a functional phosphorelay in the latter group and that the direction of phosphotransfer is reversed by cyclic di-GMP. It is important to improve understanding of more representatives of this pathway in order to obtain deeper insight into the function, composition, and evolutionary significance of a wider range of bacterial regulatory networks.

摘要

蛋白质磷酸化是原核生物和真核生物中细胞信号转导的普遍机制。组氨酸激酶 CckA、组氨酸磷酸转移酶 ChpT 和反应调节蛋白 CtrA 在整个α变形菌中是保守的。在 ,这些蛋白是基因转移剂(RcGTA)的关键调节剂,RcGTA 存在于几种α变形菌中。使用纯化的重组 蛋白,我们展示了 CckA 蛋白的自动磷酸化,以及磷酸转移到 ChpT,然后转移到 CtrA,从而在生化上证明它们形成了磷酸传递。第二信使环二鸟苷酸 (cyclic di-GMP) 将 CckA 从激酶转变为磷酸酶,导致磷酸传递在接力中逆转。CckA 中的两个残基的取代极大地影响了该蛋白的激酶或磷酸酶活性,并且突变 CckA 蛋白的产生证实了激酶但不是磷酸酶活性对于 RcGTA 的裂解释放很重要。然而,磷酸酶活性对于产生功能性 RcGTA 颗粒是必需的。使用基于生物素化环二鸟苷酸和链霉亲和素连接珠的下拉测定法直接评估了野生型和突变型 CckA 蛋白与环二鸟苷酸的结合。CckA、ChpT 和 CtrA 磷酸传递蛋白在α变形菌中广泛存在,并且有两组生物体在该途径是否对细胞存活至关重要方面存在差异。对于该途径不是必需的生物体中的这些蛋白的生化功能知之甚少,其中一组包括 这项工作在生化上证明了 CckA、ChpT 和 CtrA 也在后者群体中形成了一个功能性磷酸传递,并且环二鸟苷酸使磷酸传递方向反转。为了更深入地了解更广泛的细菌调控网络的功能、组成和进化意义,了解该途径的更多代表是很重要的。

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