首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >A secondary drug resistance mutation of TEM-1 β-lactamase that suppresses misfolding and aggregation
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A secondary drug resistance mutation of TEM-1 β-lactamase that suppresses misfolding and aggregation

机译:TEM-1β-内酰胺酶的二次耐药性突变,抑制错误折叠和聚集

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摘要

In Gram-negative bacteria. TEM-1 β-lactamase provides the major mechanism of plasmid-mediated β-lactam resistance. Natural vari- ants of TEM-1 with increased antibiotic resistance have appeared in response to the use of extended-spectrum ?-lactam antibiotics (e.g., ceftazidime) and β-lactamase inhibitors (e.g., clavulanic acid). Some of the variant enzymes are more efficient at catalyzing β-lactam hydrolysis. whereas others are more resistant to inhibi- tors. M182T is a substitution observed in both types of variant TEM-1 p-lactamases. This mutation is found only in combination with other amino acid substitutions, suggesting that it may correct defects introduced by other mutations that alter the specificity. An engineered core mutation. L76N, which diminishes the periplasmic β-lactamase activity by 100-fold, was used as a model to under- stand the mechanism of suppression of the M182T mutation. Biochemical studies of the L76N enzyme alone and in combination with the M 182T mutation indicate that the M182T substitution acts at the level of folding but does not affect the thermodynamic stability of TEM-1 β-lactamase. Thus, the M182T substitution is an example of a naturally occurring mutation that has evolved to alter the folding pathway of a protein and confer a selective advantage during the evolution of drug resistance.
机译:在革兰氏阴性细菌中。 TEM-1β-内酰胺酶提供了质粒介导的β-内酰胺抗性的主要机制。 TEM-1的天然变种具有增强的抗药性,这是由于使用了广谱的β-内酰胺类抗生素(例如头孢他啶)和β-内酰胺酶抑制剂(例如棒酸)。一些变体酶在催化β-内酰胺水解方面更有效。而其他的则更能抵抗抑制剂。 M182T是在两种类型的TEM-1对内酰胺酶变体中观察到的取代。仅与其他氨基酸取代结合发现此突变,表明它可以纠正其他改变特异性的突变所引入的缺陷。工程核心突变。 L76N可将周质β-内酰胺酶活性降低100倍,用作了解M182T突变抑制机制的模型。单独和与M 182T突变结合使用的L76N酶的生化研究表明,M182T取代在折叠水平起作用,但不影响TEM-1β-内酰胺酶的热力学稳定性。因此,M182T取代是自然发生的突变的一个例子,该突变已进化为改变蛋白质的折叠途径并在耐药性演变过程中赋予选择优势。

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