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Cholesterol sulfate as a potential inhibitor of hepatitis C virus NS3 helicase

机译:硫酸胆固醇作为丙型肝炎病毒NS3解旋酶的潜在抑制剂

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Hepatitis C virus nonstructural protein 3 (NS3) helicase is a promising target for developing new therapeutics. In this study, we identified cholesterol sulfate (CS) as a novel NS3 helicase inhibitor (IC50 = 1.7 +/- 0.2 mu M with a Hill coefficient of 3.9) by screening the extracts from marine organisms. The lack of the sulfate group, sterol structure or alkyl side chain of CS diminished the inhibition, suggesting that an anion binding and hydrophobic region in NS3 may be a target site of CS. It was further found that CS partly inhibits NS3-RNA binding activity, but exerted no or less inhibition against ATPase and serine protease activities. Moreover, we demonstrated that CS probably does not bind to RNA. Our findings suggest that CS may inhibit NS3 helicase not by abolishing the other NS3 activities but by inducing conformational changes via interaction with possible allosteric sites of NS3.
机译:丙型肝炎病毒非结构蛋白3(NS3)解旋酶是开发新疗法的有希望的目标。在这项研究中,我们通过筛选海洋生物的提取物,将硫酸胆固醇(CS)鉴定为新型NS3解旋酶抑制剂(IC50 = 1.7 +/- 0.2μM,希尔系数为3.9)。 CS的硫酸根基团,固醇结构或烷基侧链的缺乏减弱了抑制作用,表明NS3中的阴离子结合和疏水区可能是CS的靶位。进一步发现CS部分抑制NS3-RNA结合活性,但是对ATP酶和丝氨酸蛋白酶活性没有或几乎没有抑制作用。此外,我们证明了CS可能不结合RNA。我们的发现表明CS可能不是通过消除其他NS3活性而是通过与NS3可能的变构位点相互作用诱导构象变化来抑制NS3解旋酶。

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