Analysis of interaction between RNA aptamer and protein using nucleotide analogs.

S Sekiya, K Fukuda, J Hwang, N Kakiuchi, K Taira, I Kusakabe, S Nishikawa
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引用次数: 1

Abstract

Non-structural protein 3 (NS3) derived from Hepatitis C virus (HCV) is essential for viral proliferation and has two functional domains; trypsin-like serine protease and helicase. Recently we obtained three types of RNA aptamers (G9-I, -II and -III) bound to NS3 protease domain (delta NS3) by in vitro selection and confirmed their strong inhibition for protease activity. These aptamers have a common sequence, 5'-GA(A/U)UGGGAC-3', forming a loop structure by Mulfold secondary structure modeling. G9-I shows a three-way junction and G9-II and -III have four-way junction structures. To characterize the active structure of these aptamers, we applied modification interference analysis using nucleotide analogs and identified common important nucleotides in these three aptamers.

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利用核苷酸类似物分析RNA适体与蛋白质的相互作用。
源自丙型肝炎病毒(HCV)的非结构蛋白3 (NS3)对病毒增殖至关重要,具有两个功能域;胰蛋白酶样丝氨酸蛋白酶和解旋酶。最近,我们通过体外筛选获得了三种结合在NS3蛋白酶结构域(NS3 δ)上的RNA适体(G9-I、-II和-III),并证实了它们对蛋白酶活性的强烈抑制作用。这些适体具有一个共同的序列,5'-GA(a /U)UGGGAC-3',通过多重二级结构建模形成环状结构。G9-I为三向结结构,G9-II和-III为四向结结构。为了表征这些适体的活性结构,我们利用核苷酸类似物进行了修饰干扰分析,并鉴定了这三个适体中共同的重要核苷酸。
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