Analysis of aptamer binding site for HCV-NS3 protease by alanine scanning mutagenesis.

J Hwang, H Fauzi, K Fukuda, S Sekiya, N Kakiuchi, K Taira, I Kusakabe, S Nishikawa
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引用次数: 7

Abstract

Nonstructural protein 3 (NS3) of Hepatitis C virus (HCV) is a multifunctional protein and possesses protease, nucleotide triphosphatase and helicase activities. The N-terminal domain of NS3 (amino acids 1027-1218; delta NS3) has a trypsin-like protease activity and is essential for processing of viral polyprotein. Accordingly it is a potential target for anti-HCV drugs and we isolated RNA aptamers (Kd = 10 nM, Ki = 100 nM) using in vitro selection strategy. To study the interaction between delta NS3 and its aptamer, we applied alanine scanning mutagenesis and constructed seven mutant proteins at positive amino acid residues on the surface of delta NS3. Binding and inhibitory activities of the NS3 aptamer against mutant proteins were kinetically analyzed. These results clarified that especially Arg161 and Arg130 are important for interaction with the NS3 aptamer.

丙氨酸扫描诱变HCV-NS3蛋白酶适体结合位点分析。
丙型肝炎病毒(HCV)非结构蛋白3 (NS3)是一种具有蛋白酶、核苷酸三磷酸酶和解旋酶活性的多功能蛋白。NS3氨基酸1027-1218的n端结构域;NS3具有胰蛋白酶样蛋白酶活性,对病毒多蛋白的加工至关重要。因此,它是抗hcv药物的潜在靶点,我们使用体外选择策略分离RNA适配体(Kd = 10 nM, Ki = 100 nM)。为了研究delta NS3与其适体之间的相互作用,我们采用丙氨酸扫描诱变技术,在delta NS3表面的正氨基酸残基上构建了7个突变蛋白。动力学分析了NS3适体对突变蛋白的结合和抑制活性。这些结果明确了Arg161和Arg130在与NS3适体的相互作用中是重要的。
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