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建模化学趋性揭示了反向磷酸转移和双功能激酶-磷酸酶的作用。

Modeling chemotaxis reveals the role of reversed phosphotransfer and a bi-functional kinase-phosphatase.

机构信息

Centre for Mathematical Biology, Mathematical Institute, University of Oxford, Oxford, United Kingdom.

出版信息

PLoS Comput Biol. 2010 Aug 19;6(8):e1000896. doi: 10.1371/journal.pcbi.1000896.

Abstract

Understanding how multiple signals are integrated in living cells to produce a balanced response is a major challenge in biology. Two-component signal transduction pathways, such as bacterial chemotaxis, comprise histidine protein kinases (HPKs) and response regulators (RRs). These are used to sense and respond to changes in the environment. Rhodobacter sphaeroides has a complex chemosensory network with two signaling clusters, each containing a HPK, CheA. Here we demonstrate, using a mathematical model, how the outputs of the two signaling clusters may be integrated. We use our mathematical model supported by experimental data to predict that: (1) the main RR controlling flagellar rotation, CheY(6), aided by its specific phosphatase, the bifunctional kinase CheA(3), acts as a phosphate sink for the other RRs; and (2) a phosphorelay pathway involving CheB(2) connects the cytoplasmic cluster kinase CheA(3) with the polar localised kinase CheA(2), and allows CheA(3)-P to phosphorylate non-cognate chemotaxis RRs. These two mechanisms enable the bifunctional kinase/phosphatase activity of CheA(3) to integrate and tune the sensory output of each signaling cluster to produce a balanced response. The signal integration mechanisms identified here may be widely used by other bacteria, since like R. sphaeroides, over 50% of chemotactic bacteria have multiple cheA homologues and need to integrate signals from different sources.

摘要

理解多个信号如何在活细胞中整合以产生平衡反应是生物学中的一个主要挑战。双组分信号转导途径,如细菌趋化作用,包括组氨酸蛋白激酶 (HPK) 和反应调节剂 (RR)。这些用于感知和响应环境变化。球形红杆菌具有复杂的化学感觉网络,包含两个信号簇,每个信号簇都包含一个 HPK,即 CheA。在这里,我们使用数学模型证明了两个信号簇的输出如何整合。我们使用数学模型和实验数据来预测:(1) 主要的 RR 控制着鞭毛的旋转,CheY(6),由其特定的磷酸酶双功能激酶 CheA(3) 辅助,作为其他 RR 的磷酸盐汇;和 (2) 涉及 CheB(2) 的磷酸接力途径将细胞质簇激酶 CheA(3)与极性定位激酶 CheA(2)连接起来,并允许 CheA(3)-P 磷酸化非同源趋化性 RR。这两种机制使 CheA(3) 的双功能激酶/磷酸酶活性能够整合并调整每个信号簇的感官输出,以产生平衡反应。这里确定的信号整合机制可能被其他细菌广泛使用,因为像 R. sphaeroides 一样,超过 50%的趋化性细菌具有多个 cheA 同源物,需要整合来自不同来源的信号。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b45a/2924250/99e6cdabaf66/pcbi.1000896.g001.jpg

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