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首页> 外文期刊>Journal of Medicinal Chemistry >Novel Approach for Linking Genotype to Phenotype in Vitro by Exploiting an Extremely Strong Interaction between RNA and Protein
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Novel Approach for Linking Genotype to Phenotype in Vitro by Exploiting an Extremely Strong Interaction between RNA and Protein

机译:通过利用RNA和蛋白质之间的极强相互作用,将基因型与表型体外连接的新方法

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We recently isolated an aptamer that binds to the Tat protein of HIV-1 with extremely high affinity and specificity (Yamamoto, R.; et al. Genes Cells 2000, 5, 371.). In the present study, we exploited this strong binding to develop a novel coupling method that links genotype with phenotype. To strengthen the original RNA-protein interaction still further, we connected three units of the aptamer in tandem and three units of a peptide derived from Tat that interacted with the aptamer. The binding of the resultant RNA, which consisted of three units of the aptamer, to the resultant peptide, which consisted of three units of the peptide, was extremely strong. In fact, the RNA-protein interaction was one of the strongest ever reported, with an apparent K_d below 16 pM. This strong interaction was attempted for the selection of functional proteins, namely, dihydrofolate reductase (DHFR) or streptavidin, which we chose as an example, and we succeeded in the expected selection, although to a limited extent, of the target protein. The noncovalent but strong interaction described above should be useful as a novel tool for the future selection of functional proteins from pools of random sequences of amino acids.
机译:我们最近分离出了以极高的亲和力和特异性与HIV-1的Tat蛋白结合的适体(Yamamoto,R .; et al.Genes Cells 2000,5,371.)。在本研究中,我们利用这种强结合来开发一种将基因型与表型联系起来的新型偶联方法。为了进一步加强原始的RNA-蛋白质相互作用,我们串联连接了三个单元的适体和三个单元的衍生自Tat的肽与适体相互作用。由三个单元的适体组成的所得RNA与由三个单元的肽组成的所得肽的结合非常牢固。实际上,RNA-蛋白质相互作用是有史以来最强的相互作用之一,其表观K_d低于16 pM。尝试这种强相互作用来选择功能蛋白,即我们选择的二氢叶酸还原酶(DHFR)或抗生蛋白链菌素,尽管在有限的程度上,我们还是成功地预期了目标蛋白的选择。上述非共价但强烈的相互作用应该用作将来从氨基酸随机序列库中选择功能蛋白的新型工具。

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