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首页> 外文期刊>Future microbiology >New inhibitors of chorismate synthase present antifungal activity against Paracoccidioides brasiliensis
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New inhibitors of chorismate synthase present antifungal activity against Paracoccidioides brasiliensis

机译:Chorismate合成酶的新抑制剂对帕拉克肽的抗真菌活性存在抗真菌活性Brasiliensis

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Aim: A structural model of chorismate synthase (CS) from the pathogenic fungus Candida albicans was used for virtual screening simulations. Methods: Docking, molecular dynamics, cell growth inhibition and protein binding assays were used for search and validation. Results: Two molecules termed CS8 and CaCS02 were identified. Further studies of the minimal inhibitory concentration demonstrated fungicidal activity against Paracoccidioides brasiliensis with a minimal inhibitory concentration and minimal fungicidal concentration of 512 and 32 mu g.ml(-1) for CS8 and CaCS02, respectively. In addition, CaCS02 showed a strong synergistic effect in combination with amphotericin B without cytotoxic effects. In vitro studies using recombinant CS from P. brasiliensis showed IC50 of 29 mu M for CaCS02 supporting our interpretation that inhibition of CS causes the observed fungicidal activity.
机译:目的:来自致病性真菌念珠菌念珠菌的融合酶合酶(CS)的结构模型用于虚拟筛选模拟。 方法:对接,分子动力学,细胞生长抑制和蛋白质结合测定用于搜索和验证。 结果:鉴定了两个称为CS8和CACSO 2的分子。 对最小抑制浓度的进一步研究将杀灭杀螨剂活性与帕拉基肽的杀菌剂活性相对于CS8和CACSO 2的最小抑制浓度和最小的杀真菌浓度为512和32μgmml(-1)。 此外,Cacs02表现出强烈的协同效应与无细胞毒性作用的两性蛋白B组合。 使用来自P. Brasiliensis的重组Cs的体外研究表明,对于CACSO 2,CACS02的IC50为29μm,支持我们的解释,抑制Cs导致观察到的杀真菌活性。

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