Merck Research Laboratories, Kenilworth, New Jersey 07033, USA.
Merck Research Laboratories, West Point, Pennsylvania 19486, USA.
Nature. 2015 Oct 29;526(7575):672-7. doi: 10.1038/nature15542. Epub 2015 Sep 30.
Riboswitches are non-coding RNA structures located in messenger RNAs that bind endogenous ligands, such as a specific metabolite or ion, to regulate gene expression. As such, riboswitches serve as a novel, yet largely unexploited, class of emerging drug targets. Demonstrating this potential, however, has proven difficult and is restricted to structurally similar antimetabolites and semi-synthetic analogues of their cognate ligand, thus greatly restricting the chemical space and selectivity sought for such inhibitors. Here we report the discovery and characterization of ribocil, a highly selective chemical modulator of bacterial riboflavin riboswitches, which was identified in a phenotypic screen and acts as a structurally distinct synthetic mimic of the natural ligand, flavin mononucleotide, to repress riboswitch-mediated ribB gene expression and inhibit bacterial cell growth. Our findings indicate that non-coding RNA structural elements may be more broadly targeted by synthetic small molecules than previously expected.
Riboswitches 是位于信使 RNA 中的非编码 RNA 结构,可与内源性配体(如特定代谢物或离子)结合,从而调节基因表达。因此,Riboswitches 是一类新颖但尚未得到充分利用的新兴药物靶标。然而,证明这一潜力是困难的,并且仅限于结构相似的抗代谢物和配体的半合成类似物,因此极大地限制了对这些抑制剂的化学空间和选择性的追求。在这里,我们报告了 ribocil 的发现和表征,它是细菌核黄素 riboswitches 的高度选择性化学调节剂,它是在表型筛选中鉴定出来的,作为天然配体黄素单核苷酸的结构上不同的合成模拟物,可抑制 riboswitch 介导的 ribB 基因表达并抑制细菌细胞生长。我们的研究结果表明,非编码 RNA 结构元件可能比以前预期的更广泛地被合成小分子靶向。
