合成和立体特异性的 4,5-取代恶唑烷酮配体结合 T 框 RNA 核糖体开关。
Synthesis and stereospecificity of 4,5-disubstituted oxazolidinone ligands binding to T-box riboswitch RNA.
机构信息
Department of Chemistry and Biochemistry, Ohio University, Athens, Ohio 45701, United States.
出版信息
J Med Chem. 2011 Oct 13;54(19):6786-95. doi: 10.1021/jm2006904. Epub 2011 Aug 31.
Abstract
The enantiomers and the cis isomers of two previously studied 4,5-disubstituted oxazolidinones have been synthesized, and their binding to the T-box riboswitch antiterminator model RNA has been investigated in detail. Characterization of ligand affinities and binding site localization indicates that there is little stereospecific discrimination for binding antiterminator RNA alone. This binding similarity between enantiomers is likely due to surface binding, which accommodates ligand conformations that result in comparable ligand-antiterminator contacts. These results have significant implications for T-box antiterminator-targeted drug discovery and, in general, for targeting other medicinally relevant RNA that do not present deep binding pockets.
摘要
已经合成了两种先前研究过的 4,5-取代恶唑烷酮的对映异构体和顺式异构体,并详细研究了它们与 T 框核糖体开关终止子模型 RNA 的结合。配体亲和力和结合位点定位的特征表明,单独结合终止子 RNA 时几乎没有立体选择性。这种对映异构体之间的结合相似性可能是由于表面结合所致,该结合可以容纳导致类似配体-终止子相互作用的配体构象。这些结果对 T 框终止子靶向药物发现具有重要意义,并且通常对靶向其他没有深结合口袋的医学相关 RNA 具有重要意义。
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