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Efficient Synthesis of Peptide and Protein Functionalized Pyrrole-Imidazole Polyamides Using Native Chemical Ligation

机译:使用天然化学连接高效合成肽和蛋白质功能化的吡咯-咪唑聚酰胺

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The advancement of DNA-based bionanotechnology requires efficient strategies to functionalize DNA nanostructures in a specific manner with other biomolecules, most importantly peptides and proteins. Common DNA-functionalization methods rely on laborious and covalent conjugation between DNA and proteins or peptides. Pyrrole-imidazole (Py–Im) polyamides, based on natural minor groove DNA-binding small molecules, can bind to DNA in a sequence specific fashion. In this study, we explore the use of Py–Im polyamides for addressing proteins and peptides to DNA in a sequence specific and non-covalent manner. A generic synthetic approach based on native chemical ligation was established that allows efficient conjugation of both peptides and recombinant proteins to Py–Im polyamides. The effect of Py–Im polyamide conjugation on DNA binding was investigated by Surface Plasmon Resonance (SPR). Although the synthesis of different protein-Py–Im-polyamide conjugates was successful, attenuation of DNA affinity was observed, in particular for the protein-Py–Im-polyamide conjugates. The practical use of protein-Py–Im-polyamide conjugates for addressing DNA structures in an orthogonal but non-covalent manner, therefore, remains to be established.
机译:基于DNA的生物纳米技术的发展需要有效的策略,以特定的方式将DNA纳米结构与其他生物分子(最重要的是肽和蛋白质)功能化。常见的DNA功能化方法依赖于DNA与蛋白质或肽之间费力且共价的结合。吡咯-咪唑(Py–Im)聚酰胺基于天然的小沟DNA结合小分子,可以以序列特异性方式结合到DNA。在这项研究中,我们探索使用Py–Im聚酰胺以序列特异性和非共价方式将蛋白质和肽定位到DNA。建立了一种基于天然化学连接的通用合成方法,该方法可以使肽和重组蛋白与Py-Im聚酰胺有效结合。表面等离子体共振(SPR)研究了Py-Im聚酰胺结合对DNA结合的影响。尽管成功合成了不同的蛋白质-Py-Im-聚酰胺共轭物,但观察到DNA亲和力减弱,尤其是蛋白质-Py-Im-聚酰胺共轭物。因此,蛋白质-Py-Im-聚酰胺共轭物以正交但非共价的方式处理DNA结构的实际应用仍有待建立。

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