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首页> 外文期刊>FEMS Microbiology Letters >ATP synthase in slow- and fast-growing mycobacteria is active in ATP synthesis and blocked in ATP hydrolysis direction
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ATP synthase in slow- and fast-growing mycobacteria is active in ATP synthesis and blocked in ATP hydrolysis direction

机译:缓慢和快速增长的分枝杆菌中的ATP合酶在ATP合成中具有活性,并在ATP水解方向上受阻

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摘要

ATP synthase is a validated drug target for the treatment of tuberculosis, and ATP synthase inhibitors are promising candidate drugs for the treatment of infections caused by other slow-growing mycobacteria, such as Mycobacterium leprae and Mycobacterium ulcerans. ATP synthase is an essential enzyme in the energy metabolism of Mycobacterium tuberculosis; however, no biochemical data are available to characterize the role of ATP synthase in slow-growing mycobacterial strains. Here, we show that inverted membrane vesicles from the slow-growing model strain Mycobacterium bovis BCG are active in ATP synthesis, but ATP synthase displays no detectable ATP hydrolysis activity and does not set up a proton-motive force (PMF) using ATP as a substrate. Treatment with methanol as well as PMF activation unmasked the ATP hydrolysis activity, indicating that the intrinsic subunit ε and inhibitory ADP are responsible for the suppression of hydrolytic activity. These results suggest that the enzyme is needed for the synthesis of ATP, not for the maintenance of the PMF. For the development of new antimycobacterial drugs acting on ATP synthase, screening for ATP synthesis inhibitors, but not for ATP hydrolysis blockers, can be regarded as a promising strategy.
机译:ATP合酶是经过验证的治疗结核病的药物靶标,ATP合酶抑制剂是有希望的候选药物,用于治疗其他缓慢增长的分枝杆菌引起的感染,例如麻风分枝杆菌和溃疡分枝杆菌。 ATP合酶是结核分枝杆菌能量代谢中必不可少的酶。但是,尚无生化数据来表征ATP合酶在缓慢生长的分枝杆菌菌株中的作用。在这里,我们显示慢速生长的模型菌株牛分枝杆菌BCG的倒膜小泡在ATP合成中很活跃,但是ATP合酶没有显示可检测到的ATP水解活性,并且没有建立使用ATP作为酶的质子动力(PMF)。基质。用甲醇处理以及PMF活化可以掩盖ATP的水解活性,表明内在的亚基ε和抑制性ADP可以抑制水解活性。这些结果表明该酶是ATP合成所必需的,而不是维持PMF所必需的。对于开发作用于ATP合酶的新型抗分枝杆菌药物,筛选ATP合成抑制剂而不是ATP水解阻滞剂可被视为一种有前途的策略。

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