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Identification of Ligand Analogs that Control c-di-GMP Riboswitches

机译:配体类似物的识别该对照C二叔Gmp核糖开关

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摘要

Riboswitches for the bacterial second messenger c-di-GMP control the expression of genes involved in numerous cellular processes such as virulence, competence, biofilm formation and flagella synthesis. Therefore, the two known c-di-GMP riboswitch classes represent promising targets for developing novel modulators of bacterial physiology. Here, we examine the binding characteristics of circular and linear c-di-GMP analogs for representatives of both class I and II c-di-GMP riboswitches derived from the pathogenic bacterium Vibrio choleae (class I) and Clostridium difficile (class II). Some compounds exhibit values for apparent dissociation constant (KD) below 1 μM and associate with riboswitch RNAs during transcription with a speed that is sufficient to influence riboswitch function. These findings are consistent with the published structural models for these riboswitches and suggest that large modifications at various positions on the ligand can be made to create novel compounds that target c-di-GMP riboswitches. Moreover, we demonstrate the potential of an engineered allosteric ribozyme for the rapid screening of chemical libraries for compounds that bind c-di-GMP riboswitches.
机译:用于细菌第二信使C-Di-GMP的核糖接口控制涉及许多细胞过程的基因的表达,如毒力,能力,生物膜形成和鞭毛合成。因此,这两种已知的C-Di-GMP核素类别代表了开发细菌生理学新型调节剂的有希望的目标。在此,我们研究源自致病菌弧菌(I类)和梭菌差异(II类)的I类和II C-DI-GMP核糖核糖开关的圆形和线性C-DI-GMP类似物的结合特征。一些化合物表现出明显的解离常数(Kd)的值,低于1μm,并在转录期间与足以影响Riboswitch函数的速度的转录期间与Riboswitch RNA相关联。这些发现与这些核糖开关的公开结构模型一致,并表明可以使配体上各种位置进行大的修饰,以产生靶向C-DI-GMP核糖开关的新化合物。此外,我们证明了用于快速筛选化学文库的工程变构核酶的潜力,用于结合C-DI-GMP核糖纤维开关的化合物。

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