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首页> 外文期刊>Journal of Molecular Modeling >Homology modelling of 3-oxoacyl-acyl carrier protein synthase II from Mycobacterium tuberculosis H37Rv and molecular docking for exploration of drugs
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Homology modelling of 3-oxoacyl-acyl carrier protein synthase II from Mycobacterium tuberculosis H37Rv and molecular docking for exploration of drugs

机译:结核分枝杆菌H37Rv中3-氧代酰基-酰基载体蛋白合酶II的同源性建模及药物研究的分子对接

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摘要

Fatty acid synthesis is essential for cell growth and viability. The 3-oxoacyl-acyl carrier protein synthase II (KAS II) from Mycobacterium tuberculosis catalyses initiation of the fatty acid synthesis pathway by condensation of acyl CoA and mycolic acid during the elongation phase. KAS II is a key regulator of bacterial fatty acid synthesis, and a promising target in the search for potent antibacterial drugs. Homology modelling was used to generate the 3-D protein structure using the known crystal structure, and the stereochemical quality of KAS II was validated. Effective drugs were selected that target the active amino acid residues of KAS II. The drugs thiolactomycin, thiophenone and the multidrug cerulenin isoniazed were found to be more potent for inhibition of M. tuberculosis due to the robust binding affinity of their protein–drug interactions. KAS II enzymes of M. tuberculosis and other species of Mycobacterium are conserved, as revealed by their close phylogenetic relationships. This study may provide new insights towards understanding the 3-D structural conformation and active amino acids of KAS II, thus providing rationale for the design of novel antibacterial drugs.
机译:脂肪酸合成对于细胞生长和活力至关重要。结核分枝杆菌的3-氧代酰基-酰基载体蛋白合酶II(KAS II)在延长阶段通过酰基辅酶A和霉菌酸的缩合催化脂肪酸合成途径的启动。 KAS II是细菌脂肪酸合成的关键调节剂,也是寻找有效抗菌药物的有希望的目标。使用同源性建模使用已知的晶体结构生成3-D蛋白结构,并验证了KAS II的立体化学质量。选择靶向KAS II的活性氨基酸残基的有效药物。由于它们的药物-药物相互作用具有很强的结合亲和力,因此发现硫代催乳素,噻吩和异烟肼的多药性蓝绿色素对结核分枝杆菌的抑制作用更强。结核分枝杆菌和其他分枝杆菌的KAS II酶是保守的,正如它们密切的系统发育关系所揭示。这项研究可能为了解KAS II的3-D结构构象和活性氨基酸提供新的见识,从而为新型抗菌药物的设计提供了依据。

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