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用于研究核酸与NCp7相互作用的含荧光吖啶的HIV-1核衣壳蛋白的合成及生物活性

Synthesis and biological activities of fluorescent acridine-containing HIV-1 nucleocapsid proteins for investigation of nucleic acid-NCp7 interactions.

作者信息

Dong C Z, De Rocquigny H, Rémy E, Mellac S, Fournié-Zaluski M C, Roques B P

机构信息

Département de Pharmacochimie Moléculaire et Structurale, INSERM U266-CNRS URA D 1500, UFR des Sciences Pharmaceutiques et Biologiques, Paris, France.

出版信息

J Pept Res. 1997 Oct;50(4):269-78. doi: 10.1111/j.1399-3011.1997.tb01468.x.

DOI:10.1111/j.1399-3011.1997.tb01468.x
PMID:9352465
Abstract

Specific interactions between the 72-amino acid nucleocapsid protein NCp7 of the human immunodeficiency virus, type 1 and the genomic RNA are essential for virus replication. Studies on the mechanism of action of NCp7 require a direct visualization of its complexes with nucleic acids and the determination of binding affinities. To facilitate these investigations, fluorescent NCp7 derivatives were developed by introduction in the NCp7 sequence of a non-natural amino acid, (S)-beta-(9-acridinyl)alanine (Aca) obtained by a chiral synthetic method. Three fluorescent NCp7 derivatives were obtained by introducing this amino acid at different positions. As shown by NMR, the three-dimensional structure of NCp7 is not altered by introduction of Aca. The fluorescent peptides were found to be as potent as their precursors in interacting with nucleic acids and in promoting HIV-1 genomic RNA dimerization. Moreover, because of their fluorescent properties, these NCp7s can be used at submicromolar concentrations to directly visualize and quantify protein-nucleic acid interactions in solution or after gel electrophoresis. This could facilitate the development of new antiviral agents aimed at inhibiting the functions of NCp7 and studies on the intracellular traffic of NCp7 within the preintegration complex.

摘要

人类免疫缺陷病毒1型(HIV-1)的72个氨基酸的核衣壳蛋白NCp7与基因组RNA之间的特异性相互作用对于病毒复制至关重要。对NCp7作用机制的研究需要直接观察其与核酸的复合物并确定结合亲和力。为便于这些研究,通过手性合成方法获得的非天然氨基酸(S)-β-(9-吖啶基)丙氨酸(Aca)引入NCp7序列,从而开发出荧光NCp7衍生物。通过在不同位置引入这种氨基酸获得了三种荧光NCp7衍生物。如核磁共振(NMR)所示,引入Aca不会改变NCp7的三维结构。发现这些荧光肽在与核酸相互作用以及促进HIV-1基因组RNA二聚化方面与其前体一样有效。此外,由于它们的荧光特性,这些NCp7可以在亚微摩尔浓度下用于直接观察和定量溶液中或凝胶电泳后的蛋白质-核酸相互作用。这有助于开发旨在抑制NCp7功能的新型抗病毒药物以及研究整合前复合物中NCp7的细胞内运输。

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