> An Asinex Gold Platinium chemical library subset of 12?055 compounds was screened employing docking simulations in '/> Identification of novel antilipogenic agents targeting fatty acid biosynthesis through structure‐based virtual screening
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Identification of novel antilipogenic agents targeting fatty acid biosynthesis through structure‐based virtual screening

机译:通过基于结构的虚拟筛选鉴定靶向脂肪酸生物合成的新型防肝剂

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> An Asinex Gold Platinium chemical library subset of 12?055 compounds was screened employing docking simulations in the active site of the human FAS KS domain. Among them, 13 compounds were further evaluated for their ability to inhibit fatty acid biosynthesis. Four compounds were found to be active in particular ASN05064661 and ASN05374526 with IC 50 values of 6.6 and 10.5?μ m , respectively. A binding mode study was further conducted with these two compounds structurally related to benzene sulfonamide and aromatic polyamide. This study showed that they fit tightly with the active site with several interactions, notably with the key residues Cys161, His293, and His331.
机译:

ASINex金铂化学文库12?055化合物在活跃点中采用对接模拟的筛选筛选 人类 Fas ks 域。 其中,进一步评估了13种化合物以抑制脂肪酸生物合成的能力。 发现四种化合物在特定的ASN05064661和ASN05374526中是活性的,分别具有6.6和10.5Ω的 IC 50值。 通过与苯磺酰胺和芳族聚酰胺构造的这两种化合物进一步进行结合模式研究。 本研究表明,它们与活性位点紧密配合,特别是几个相互作用,特别是与关键残留物Cys161,HIS293和HIS331相互作用。

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