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Direct sensing and signal transduction during bacterial chemotaxis toward aromatic compounds in Comamonas testosteroni

机译:细菌趋化睾丸激素对芳香族化合物的趋化过程中的直接传感和信号转导

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Micro-organisms sense and chemotactically respond to aromatic compounds. Although the existence of chemoreceptors that bind to aromatic attractants and subsequently trigger chemotaxis have long been speculated, such a chemoreceptor has not been demonstrated. In this report, we demonstrated that the chemoreceptor MCP2901 from Comamonas testosteroni CNB-1 binds to aromatic compounds and initiates downstream chemotactic signaling in addition to its ability to trigger chemotaxis via citrate binding. The function of gene MCP2901 was investigated by genetic deletion from CNB-1 and genetic complementation of the methyl-accepting chemotaxis protein (MCP)-null mutant CNB-120. Results showed that the expression of MCP2901 in the MCP-null mutant restored chemotaxis toward nine tested aromatic compounds and nine carboxylic acids. Isothermal titration calorimetry (ITC) analyses demonstrated that the ligand-binding domain of MCP2901 (MCP2901LBD) bound to citrate, and weakly to gentisate and 4-hydroxybenzoate. Additionally, ITC assays indicated that MCP2901LBD bound strongly to 2,6-dihydroxybenzoate and 2-hydroxybenzoate, which are isomers of gentisate and 4-hydroxybenzoate respectively that are not metabolized by CNB-1. Agarose-in-plug and capillary assays showed that these two molecules serve as chemoattractants for CNB-1. Through constructing membrane-like MCP2901-inserted Nanodiscs and phosphorelay activity assays, we demonstrated that 2,6-dihydroxybenzoate and 2-hydroxybenzoate altered kinase activity of CheA. This is the first evidence of an MCP binding to an aromatic molecule and triggering signal transduction for bacterial chemotaxis.
机译:微生物感知并趋向于对芳香族化合物产生化学反应。尽管长期以来一直存在与芳香族引诱剂结合并随后触发趋化性的化学感受器的存在,但尚未证明这种化学感受器。在本报告中,我们证明了来自Comomonas testosteroni CNB-1的化学感受器MCP2901与芳香族化合物结合并启动下游趋化信号传递,此外还具有通过柠檬酸盐结合触发趋化作用的能力。通过从CNB-1上进行基因缺失和对甲基化趋化蛋白(MCP)无效的突变体CNB-120进行遗传互补,研究了MCP2901基因的功能。结果显示,MCP-null突变体中的MCP2901的表达恢复了对9种被测芳香族化合物和9种羧酸的趋化性。等温滴定热分析(ITC)分析表明,MCP2901(MCP2901LBD)的配体结合结构域与柠檬酸盐结合,而与龙胆酸酯和4-羟基苯甲酸酯结合较弱。此外,ITC分析表明,MCP2901LBD与2,6-二羟基苯甲酸酯和2-羟基苯甲酸酯牢固结合,后者分别是龙胆酸酯和4-羟基苯甲酸酯的异构体,不会被CNB-1代谢。琼脂糖插入法和毛细管测定法表明这两个分子充当CNB-1的化学引诱剂。通过构建膜样MCP2901插入的纳米光盘和磷灰泥活性测定,我们证明了2,6-二羟基苯甲酸酯和2-羟基苯甲酸酯改变了CheA的激酶活性。这是MCP与芳香分子结合并触发细菌趋化性信号转导的第一个证据。

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