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ATPase Activity of Mycobacterium tuberculosis SecA1 and SecA2 Proteins and Its Importance for SecA2 Function in Macrophages▿

机译:结核分枝杆菌SecA1和SecA2蛋白的ATPase活性及其对巨噬细胞中SecA2功能的重要性Import

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摘要

The Sec-dependent translocation pathway that involves the essential SecA protein and the membrane-bound SecYEG translocon is used to export many proteins across the cytoplasmic membrane. Recently, several pathogenic bacteria, including Mycobacterium tuberculosis, were shown to possess two SecA homologs, SecA1 and SecA2. SecA1 is essential for general protein export. SecA2 is specific for a subset of exported proteins and is important for M. tuberculosis virulence. The enzymatic activities of two SecA proteins from the same microorganism have not been defined for any bacteria. Here, M. tuberculosis SecA1 and SecA2 are shown to bind ATP with high affinity, though the affinity of SecA1 for ATP is weaker than that of SecA2 or Escherichia coli SecA. Amino acid substitution of arginine or alanine for the conserved lysine in the Walker A motif of SecA2 eliminated ATP binding. We used the SecA2(K115R) variant to show that ATP binding was necessary for the SecA2 function of promoting intracellular growth of M. tuberculosis in macrophages. These results are the first to show the importance of ATPase activity in the function of accessory SecA2 proteins.
机译:Sec依赖的易位途径,涉及必需的SecA蛋白和膜结合的SecYEG易位子,用于跨细胞质膜输出许多蛋白。最近,一些致病菌,包括结核分枝杆菌,被证明拥有两个SecA同源物SecA1和SecA2。 SecA1对于一般蛋白质出口至关重要。 SecA2对一部分输出蛋白具有特异性,对结核分枝杆菌毒力也很重要。尚未确定来自同一微生物的两种SecA蛋白的酶促活性。在此,结核分枝杆菌SecA1和SecA2显示出以高亲和力结合ATP,尽管SecA1对ATP的亲和力弱于SecA2或大肠杆菌SecA。 SecA2的Walker A基序中保守赖氨酸的精氨酸或丙氨酸氨基酸取代消除了ATP结合。我们使用SecA2(K115R)变体显示ATP结合对于促进巨噬细胞中结核分枝杆菌的细胞内生长的SecA2功能是必需的。这些结果是第一个显示ATPase活性在SecA2辅助蛋白功能中的重要性的研究。

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