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Inhibition of Klenow DNA polymerase and poly(A)-specific ribonuclease by aminoglycosides.

机译:氨基糖苷对Klenow DNA聚合酶和聚(A)特异性核糖核酸酶的抑制作用。

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摘要

Aminoglycosides are known to bind and perturb the function of catalytic RNA. Here we show that they also are potent inhibitors of protein-based catalysis using Escherichia coli Klenow polymerase (pol) and mammalian poly(A)-specific ribonuclease (PARN) as model enzymes. The inhibition was pH dependent and released in a competitive manner by Mg2+. Kinetic analysis showed that neomycin B behaved as a mixed noncompetitive inhibitor. Iron-mediated hydroxyl radical cleavage was used to show that neomycin B interfered with metal-ion binding in the active sites of both enzymes. Our analysis suggests a mechanism of inhibition where the aminoglycoside binds in the active site of the enzyme and thereby displaces catalytically important divalent metal ions. The potential causes of aminoglycoside toxicity and the usage of aminoglycosides to probe, characterize, and perturb metalloenzymes are discussed.
机译:已知氨基糖苷结合并干扰催化RNA的功能。在这里,我们显示它们也是使用大肠杆菌Klenow聚合酶(pol)和哺乳动物多聚(A)特异性核糖核酸酶(PARN)作为模型酶的基于蛋白质的催化的有效抑制剂。抑制作用是pH依赖性的,并且会被Mg2 +竞争性释放。动力学分析表明,新霉素B表现为混合的非竞争性抑制剂。铁介导的羟基自由基裂解被用于显示新霉素B干扰了两种酶活性位点中的金属离子结合。我们的分析提出了一种抑制机制,其中氨基糖苷结合在酶的活性位点上,从而取代了重要的催化二价金属离子。讨论了氨基糖苷毒性的潜在原因以及使用氨基糖苷来探测,表征和扰动金属酶。

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