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一种针对人乳头瘤病毒16型L1病毒样颗粒的RNA适配体的特性分析

Characterization of an RNA aptamer against HPV-16 L1 virus-like particles.

作者信息

Leija-Montoya Ana Gabriela, Benítez-Hess María Luisa, Toscano-Garibay Julia Dolores, Alvarez-Salas Luis Marat

机构信息

1 Laboratorio de Terapia Génica, Departamento de Genética y Biología Molecular, Centro de Investigación y de Estudios Avanzados del I.P.N. , México D.F., México .

出版信息

Nucleic Acid Ther. 2014 Oct;24(5):344-55. doi: 10.1089/nat.2013.0469. Epub 2014 Aug 11.

Abstract

The human papillomavirus (HPV) capsid is mainly composed of the L1 protein that can self-assemble into virus-like particles (VLPs) that are structurally and immunologically similar to the infectious virions. We report here the characterization of RNA aptamers that recognize baculovirus-produced HPV-16 L1 VLPs. Interaction and slot-blot binding assays showed that all isolated aptamers efficiently bound HPV-16 VLPs, although the Sc5-c3 aptamer showed the highest specificity and affinity (Kd=0.05 pM). Sc5-c3 secondary structure consisted of a hairpin with a symmetric bubble and an unstructured 3'end. Biochemical and genetic analyses showed that the Sc5-c3 main loop is directly involved on VLPs binding. In particular, binding specificity appeared mediated by five non-consecutive nucleotide positions. Experiments using bacterial-produced HPV-16 L1 resulted in low Sc5-c3 binding, suggesting that recognition of HPV-16 L1 VLPs relies on quaternary structure features not present in bacteria-produced L1 protein. Sc5-c3 produced specific and stable binding to HPV-16 L1 VLPs even in biofluid protein mixes and thus it may provide a potential diagnostic tool for active HPV infection.

摘要

人乳头瘤病毒(HPV)衣壳主要由L1蛋白组成,该蛋白可自组装成病毒样颗粒(VLP),其在结构和免疫方面与感染性病毒粒子相似。我们在此报告了识别杆状病毒产生的HPV - 16 L1 VLP的RNA适配体的特性。相互作用和狭缝印迹结合试验表明,所有分离出的适配体均能有效结合HPV - 16 VLP,尽管Sc5 - c3适配体显示出最高的特异性和亲和力(解离常数Kd = 0.05 pM)。Sc5 - c3二级结构由带有对称气泡的发夹结构和无结构的3'末端组成。生化和遗传学分析表明,Sc5 - c3的主要环直接参与VLP结合。特别是,结合特异性似乎由五个不连续的核苷酸位置介导。使用细菌产生的HPV - 16 L1进行的实验导致Sc5 - c3结合率较低,这表明对HPV - 16 L1 VLP的识别依赖于细菌产生的L1蛋白中不存在的四级结构特征。即使在生物流体蛋白混合物中,Sc5 - c3也能与HPV - 16 L1 VLP产生特异性和稳定的结合,因此它可能为活跃的HPV感染提供一种潜在的诊断工具。

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