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Structure-activity relationships of cryptopleurine analogs with E-ring modifications as anti-hepatitis C virus agents

机译:具有E环修饰的隐性小鸟嘌呤类似物作为抗丙型肝炎病毒制剂的构效关系

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摘要

The tylophorine analog -cryptopleurine exhibited potent anti-hepatitis C virus (HCV) activity through allosteric regulation of ATPase activity of heat shock cognate protein 70 (Hsc70). We evaluated the impact of modifications on the E-ring of -cryptopleurine to the inhibitory activity against HCV replication and regulation of ATPase activity of Hsc70. Cryptopleurine analog YXM-110 with a 13α-hydroxyl group maintained activity against HCV and promoted ATP/ADP turnover of Hsc70; however, compounds with hydroxyl groups at other positions or with other orientations (YXM-109, YXM-139, and YXM-140) did not exhibit similar activities. Size modification or heteroatom incorporation of the E-ring led to loss of anti-HCV activity. Promotion of the chaperone activity of Hsc70 with carboxyl terminus Hsc70 interacting protein (CHIP) further enhanced the anti-HCV activity of -cryptopleurine and XYM-110. This structure-activity relationship (SAR) study refined structural design and optimization for developing -crytopleurine analogs as potent anti-HCV agents targeted against the host factor involved in HCV replication.
机译:酪氨酸类似物-隐亮氨酸通过热休克同源蛋白70(Hsc70)的ATPase活性的变构调节,表现出有效的抗丙型肝炎病毒(HCV)活性。我们评估了修饰对-cryptopleurine E环的抗HCV复制和Hsc70 ATPase活性的抑制活性的影响。具有13α-羟基的隐尿嘧啶类似物YXM-110保持抗HCV活性并促进Hsc70的ATP / ADP转化。但是,在其他位置或其他方向带有羟基的化合物(YXM-109,YXM-139和YXM-140)没有表现出相似的活性。 E环的尺寸修改或杂原子掺入导致抗HCV活性丧失。用羧基末端Hsc70相互作用蛋白(CHIP)促进Hsc70的伴侣活性进一步增强了-cryptopleurine和XYM-110的抗HCV活性。这项结构与活性关系(SAR)研究改进了结构设计和优化方法,用于开发-胰亮氨酸类似物,作为针对HCV复制涉及宿主因子的有效抗HCV药物。

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