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DifA, a Methyl-Accepting Chemoreceptor Protein-Like Sensory Protein, Uses a Novel Signaling Mechanism to Regulate Exopolysaccharide Production in Myxococcus xanthus▿ †

机译:DifA,一种像甲基的化学感受器蛋白一样的感觉蛋白,使用新型的信号传导机制来调节粘多糖中的胞外多糖产生▿

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摘要

DifA is a methyl-accepting chemotaxis protein (MCP)-like sensory transducer that regulates exopolysaccharide (EPS) production in Myxococcus xanthus. Here mutational analysis and molecular biology were used to probe the signaling mechanisms of DifA in EPS regulation. We first identified the start codon of DifA experimentally; this identification extended the N terminus of DifA for 45 amino acids (aa) from the previous bioinformatics prediction. This extension helped to address the outstanding question of how DifA receives input signals from type 4 pili without a prominent periplasmic domain. The results suggest that DifA uses its N-terminus extension to sense an upstream signal in EPS regulation. We suggest that the perception of the input signal by DifA is mediated by protein-protein interactions with upstream components. Subsequent signal transmission likely involves transmembrane signaling instead of direct intramolecular interactions between the input and the output modules in the cytoplasm. The basic functional unit of DifA for signal transduction is likely dimeric as mutational alteration of the predicted dimeric interface of DifA significantly affected EPS production. Deletions of 14-aa segments in the C terminus suggest that the newly defined flexible bundle subdomain in MCPs is likely critical for DifA function because shortening of this bundle can lead to constitutively active mutations.
机译:DifA是一种甲基受体趋化蛋白(MCP)样的感官传感器,可调节黄色粘球菌中胞外多糖(EPS)的产生。在这里,突变分析和分子生物学被用来探讨DifA在EPS调节中的信号传导机制。我们首先通过实验确定了DifA的起始密码子。这项鉴定将DifA的N末端从先前的生物信息学预测扩展到45个氨基酸(aa)。此扩展帮助解决了一个悬而未决的问题,即DifA如何在没有明显的周质结构域的情况下从4型菌毛接收输入信号。结果表明,DifA使用其N端延伸来检测EPS调节中的上游信号。我们建议,DifA对输入信号的感知是通过蛋白质与上游成分之间的相互作用介导的。随后的信号传输可能涉及跨膜信号传递,而不是细胞质中输入模块和输出模块之间的直接分子内相互作用。 DifA用于信号转导的基本功能单元很可能是二聚体,因为DifA的预测二聚体界面的突变改变显着影响了EPS的产生。 C末端14-aa区段的缺失表明,MCP中新定义的柔性束亚结构域可能对DifA功能至关重要,因为缩短该束可导致组成性活性突变。

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