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氨基糖苷类对三链螺旋核酸的识别。

Recognition of triple helical nucleic acids by aminoglycosides.

作者信息

Xi H, Arya D P

机构信息

Laboratory of Medicinal Chemistry, Department of Chemistry, Clemson University, Clemson, South Carolina, 29634, USA.

出版信息

Curr Med Chem Anticancer Agents. 2005 Jul;5(4):327-38. doi: 10.2174/1568011054222328.

Abstract

Aminoglycosides, traditional RNA binders, were found to be a new class of triple helical nucleic acid-stabilizing ligands. Neomycin, of all the aminoglycosides, has shown the most significant effects in stabilizing DNA, RNA, and hybrid triple helices. When compared with minor groove binders or intercalators, neomycin excels at triple helical stabilization in most cases. Molecular modeling studies suggest that neomycin reaches into the larger Watson-Hoogsteen groove. The charge and shape complementarity are the key factors in neomycin-triplex recognition. By conjugating neomycin with intercalators such as BQQ (a potent triple helix intercalating agent designed by Hélène), we have progressed in developing more potent triple helix stabilizing ligands. The design of such dual or even triple recognition ligands opens a new paradigm for recognition of triple helix nucleic acids. The article herein presents studies of neomycin as the first molecule that can selectively stabilize nucleic acid triplex structures. These studies are supported by our recent discovery that neomycin prefers to bind to A-like conformations, of which triple helix structures are known to display some characteristics. These findings will contribute to the development of a new series of triplex-specific ligands, and may contribute to either antisense or antigene therapies.

摘要

氨基糖苷类药物作为传统的RNA结合剂,被发现是一类新型的能稳定三链核酸的配体。在所有氨基糖苷类药物中,新霉素在稳定DNA、RNA和杂交三链螺旋方面显示出最显著的效果。与小沟结合剂或嵌入剂相比,新霉素在大多数情况下在稳定三链螺旋方面表现出色。分子模拟研究表明,新霉素进入较大的沃森-霍格施泰因沟。电荷和形状互补性是新霉素与三链体识别的关键因素。通过将新霉素与嵌入剂如BQQ(由埃莱娜设计的一种有效的三链螺旋嵌入剂)偶联,我们在开发更有效的三链螺旋稳定配体方面取得了进展。这种双重甚至三重识别配体的设计为识别三链螺旋核酸开辟了新的范例。本文介绍了将新霉素作为第一个能选择性稳定核酸三链体结构的分子的研究。我们最近发现新霉素更喜欢与A样构象结合,而三链螺旋结构已知具有一些该构象的特征,这些研究得到了这一发现的支持。这些发现将有助于开发一系列新的三链体特异性配体,并可能有助于反义或反基因治疗。

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