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由双环-C残基稳定的DNA双链体的晶体结构。

Crystal structures of DNA duplexes stabilized by bicyclic-C residues.

作者信息

Haraguchi Tsuyoshi, Shimizu Satoru, Ma Xiao, Kurose Taizo, Juan Ella Czarina Magat, Ohkubo Akihiro, Sekine Mitsuo, Shibata Takayuki, Millington Christopher L, Williams David M, Takénaka Akio

机构信息

Graduate School of Bioscience and Biotechnology, Tokyo Institute of Technology, Yokohama 226-8501, Japan.

出版信息

Nucleic Acids Symp Ser (Oxf). 2008(52):127-8. doi: 10.1093/nass/nrn065.

Abstract

Chemical modification of nucleic acids is being studied extensively as an approach for the development of nucleic acid-based therapies. We found that a nucleotide carrying 7,8-dihydropyrido[2,3-d]pyrimidin-2-one (bicyclic-C or X), which is a cytosine derivative with a propene attached at the N4 and C5 atoms, increases the stability of DNA duplexes. To establish the conformational effects of X on DNA and to obtain insight into the correlation between the structure and stability of X-containing DNA duplexes, the crystal structures of d(CGCGAATT-X-GCG) and d(CGCGAAT-X-CGCG) have been determined at 2.9 A resolutions. In both duplexes, the bicyclic-C bases form pairs with the counter bases through hydrogen bonds, and stabilize the duplex formation in part by stacking interactions between X and the subsequent thymine base of the same strand.

摘要

核酸的化学修饰作为一种基于核酸疗法的开发方法正在被广泛研究。我们发现,携带7,8 - 二氢吡啶并[2,3 - d]嘧啶 - 2 - 酮(双环 - C或X)的核苷酸,它是一种胞嘧啶衍生物,在N4和C5原子处连接有丙烯,可增加DNA双链体的稳定性。为了确定X对DNA的构象影响,并深入了解含X的DNA双链体的结构与稳定性之间的相关性,已在2.9埃分辨率下测定了[d(CGCGAATT - X - GCG)]₂和[d(CGCGAAT - X - CGCG)]₂的晶体结构。在这两种双链体中,双环 - C碱基通过氢键与互补碱基形成配对,并部分通过X与同一条链上随后的胸腺嘧啶碱基之间的堆积相互作用来稳定双链体的形成。

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