DNA 回旋酶和拓扑异构酶 IV 的双重靶向:金黄色葡萄球菌中杂芳基异噻唑啉酮的靶点相互作用
Dual targeting of DNA gyrase and topoisomerase IV: target interactions of heteroaryl isothiazolones in Staphylococcus aureus.
作者信息
Cheng Jijun, Thanassi Jane A, Thoma Christy L, Bradbury Barton J, Deshpande Milind, Pucci Michael J
机构信息
Achillion Pharmaceuticals, New Haven, CT 06511, USA.
出版信息
Antimicrob Agents Chemother. 2007 Jul;51(7):2445-53. doi: 10.1128/AAC.00158-07. Epub 2007 May 14.
Heteroaryl isothiazolones (HITZs) are antibacterial agents that display excellent in vitro activity against Staphylococcus aureus. We recently identified a series of these compounds that show potent bactericidal activities against methicillin-resistant Staphylococcus aureus (MRSA). We report here the results of in vitro resistance studies that reveal potential underlying mechanisms of action. HITZs selected gyrA mutations exclusively in first-step mutants of wild-type S. aureus, indicating that in contrast to the case with most quinolones, DNA gyrase is the primary target. The compounds displayed low mutation frequencies (10(-9) to 10(-10)) at concentrations close to the MICs and maintained low MICs (< or =0.016 microg/ml) against mutants with single mutations in either gyrA or grlA (parC). These data suggested that HITZs possess significant inhibitory activities against target enzymes, DNA gyrase and topoisomerase IV. This dual-target inhibition was supported by low 50% inhibitory concentrations against topoisomerase IV as measured in a decatenation activity assay and against DNA gyrase as measured in a supercoiling activity assay. Good antibacterial activities (< or =1 microg/ml) against staphylococcal gyrA grlA double mutants, as well as low frequencies (10(-9) to 10(-10)) of selection of still higher-level mutants, also suggested that HITZs remained active against mutant enzymes. We further demonstrated that HITZs exhibit good inhibition of both S. aureus mutant enzymes and thus continue to possess a novel dual-targeting mode of action against these mutant strains. In stepwise acquisition of mutations, HITZs selected quinolone resistance determining region mutations gyrA(Ser84Leu), grlA(Ser80Phe), grlA(Ala116Val), and gyrA(Glu88Lys) sequentially, suggesting that the corresponding amino acids are key amino acids involved in the binding of HITZs to topoisomerases. The overall profile of these compounds suggests the potential utility of HITZs in combating infections caused by S. aureus, including multidrug-resistant MRSA.
杂芳基异噻唑啉酮(HITZs)是一类抗菌剂,对金黄色葡萄球菌具有出色的体外活性。我们最近鉴定出一系列此类化合物,它们对耐甲氧西林金黄色葡萄球菌(MRSA)表现出强大的杀菌活性。我们在此报告体外耐药性研究的结果,这些结果揭示了潜在的作用机制。HITZs仅在野生型金黄色葡萄球菌的第一步突变体中选择gyrA突变,这表明与大多数喹诺酮类药物的情况不同,DNA回旋酶是主要靶点。这些化合物在接近最低抑菌浓度(MIC)的浓度下显示出低突变频率(10^(-9)至10^(-10)),并且对gyrA或grlA(parC)中单个突变的突变体保持低MIC(≤0.016μg/ml)。这些数据表明HITZs对靶酶DNA回旋酶和拓扑异构酶IV具有显著的抑制活性。在解连环活性测定中对拓扑异构酶IV以及在超螺旋活性测定中对DNA回旋酶测得的低50%抑制浓度支持了这种双靶点抑制作用。对葡萄球菌gyrA grlA双突变体具有良好的抗菌活性(≤1μg/ml),以及选择更高水平突变体的低频率(10^(-9)至10^(-10)),也表明HITZs对突变酶仍然具有活性。我们进一步证明,HITZs对金黄色葡萄球菌突变酶均表现出良好的抑制作用,因此继续对这些突变菌株具有一种新型的双靶点作用模式。在逐步获得突变的过程中,HITZs依次选择喹诺酮耐药决定区突变gyrA(Ser84Leu)、grlA(Ser80Phe)、grlA(Ala116Val)和gyrA(Glu88Lys),这表明相应的氨基酸是参与HITZs与拓扑异构酶结合的关键氨基酸。这些化合物的总体情况表明HITZs在对抗由金黄色葡萄球菌引起的感染(包括多重耐药的MRSA)方面具有潜在用途。
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