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首页> 外文期刊>FEBS letters. >Tyrosine partners coordinate DNA nicking by the Salmonella typhimurium plasmid pCU1 relaxase enzyme.
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Tyrosine partners coordinate DNA nicking by the Salmonella typhimurium plasmid pCU1 relaxase enzyme.

机译:酪氨酸伴侣通过鼠伤寒沙门氏菌质粒pCU1松弛酶来协调DNA切割。

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摘要

Conjugative plasmid transfer results in the spread of antibiotic resistance genes and virulence factors between bacterial cells. Plasmid transfer is dependent upon the DNA nicking activity of a plasmid-encoded relaxase enzyme. Tyrosine residues within the relaxase cleave the DNA plasmid nic site in a highly sequence-specific manner. The conjugative resistance plasmid pCU1 encodes a relaxase with four tyrosine residues surrounding its active site (Y18,19,26,27). We use activity assays to demonstrate that the pCU1 relaxase preferentially uses Y26 or a combination of Y18 + 19 to nick DNA at wild type levels, and that an adjacent aspartic acid deprotonates these tyrosines to activate them for attack. Our findings illustrate the unique modifications that the pCU1 relaxase has introduced into the traditional relaxase-mediated DNA nicking mechanism.
机译:结合质粒转移导致抗生素抗性基因和毒力因子在细菌细胞之间扩散。质粒转移取决于质粒编码的松弛酶的DNA切口活性。松弛酶内的酪氨酸残基以高度序列特异性的方式切割DNA质粒nic位点。结合抗性质粒pCU1编码一个松弛酶,在其活性位点周围有四个酪氨酸残基(Y18、19、26、27)。我们使用活性测定法证明pCU1松弛酶优先使用Y26或Y18 + 19的组合在野生型水平上刻划DNA,并且相邻的天冬氨酸使这些酪氨酸去质子化以激活它们进行攻击。我们的发现说明了pCU1松弛酶已引入传统的松弛酶介导的DNA切口机制的独特修饰。

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