首页> 外文期刊>Journal of bacteriology >Redundant Function of cmaA2 and mmaA2 in Mycobacterium tuberculosis cis Cyclopropanation of Oxygenated Mycolates
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Redundant Function of cmaA2 and mmaA2 in Mycobacterium tuberculosis cis Cyclopropanation of Oxygenated Mycolates

机译:cmaA2和mmaA2在结核分枝杆菌顺式环丙烷氧化的霉菌酸酯中的冗余功能

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The Mycobacterium tuberculosis cell envelope contains a wide variety of lipids and glycolipids, including mycolic acids, long-chain branched fatty acids that are decorated by cyclopropane rings. Genetic analysis of the mycolate methyltransferase family has been a powerful approach to assign functions to each of these enzymes but has failed to reveal the origin of cis cyclopropanation of the oxygenated mycolates. Here we examine potential redundancy between mycolic acid methyltransferases by generating and analyzing M. tuberculosis strains lacking mmaA2 and cmaA2, mmaA2 and cmaA1, or mmaA1 alone. M. tuberculosis lacking both cmaA2 and mmaA2 cannot cis cyclopropanate methoxymycolates or ketomycolates, phenotypes not shared by the mmaA2 and cmaA2 single mutants. In contrast, a combined loss of cmaA1 and mmaA2 had no effect on mycolic acid modification compared to results with a loss of mmaA2 alone. Deletion of mmaA1 from M. tuberculosis abolishes trans cyclopropanation without accumulation of trans-unsaturated oxygenated mycolates, placing MmaA1 in the biosynthetic pathway for trans-cyclopropanated oxygenated mycolates before CmaA2. These results define new functions for the mycolic acid methyltransferases of M. tuberculosis and indicate a substantial redundancy of function for MmaA2 and CmaA2, the latter of which can function as both a cis and trans cyclopropane synthase for the oxygenated mycolates.
机译:结核分枝杆菌细胞包膜含有多种脂质和糖脂,包括霉菌酸,被环丙烷环修饰的长链支链脂肪酸。霉菌酸酯甲基转移酶家族的遗传分析是将功能分配给这些酶的一种有效方法,但未能揭示含氧霉菌酸酯的顺式环丙烷化的起源。在这里,我们通过生成和分析M来检查霉菌酸甲基转移酶之间的潜在冗余。缺乏 mmaA2 cmaA2 mmaA2 cmaA1 mmaA1 的结核菌株em>一个人。 M。缺乏 cmaA2 mmaA2 的肺结核不能顺式环丙酸酯甲氧基霉菌酸酯或酮霉菌酸酯,这些表型不是 mmaA2 cmaA2 单个突变体。相反,与 mmaA2 单独损失相比, cmaA1 mmaA2 的综合损失对霉菌酸修饰没有影响。从 M中删除 mmaA1 。结核病消除了 trans 的环丙烷化,而没有 trans -不饱和的氧化霉菌酸酯的积累,将MmaA1置于 trans -环丙烷化的氧化霉菌酸酯的生物合成途径中。在CmaA2之前。这些结果定义了 M的霉菌酸甲基转移酶的新功能。结核病,表明MmaA2和CmaA2的功能存在大量冗余,后者对于氧化的霉菌酸酯可同时充当 cis trans 环丙烷合酶。

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