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Translational regulation by bacterial small RNAs via an unusual Hfq-dependent mechanism

机译:细菌小RNA通过不寻常的Hfq依赖机制进行翻译调控

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摘要

In bacteria, the canonical mechanism of translational repression by small RNAs (sRNAs) involves sRNA-mRNA base pairing that occludes the ribosome binding site (RBS), directly preventing translation. In this mechanism, the sRNA is the direct regulator, while the RNA chaperone Hfq plays a supporting role by stabilizing the sRNA. There are a few examples where the sRNA does not directly interfere with ribosome binding, yet translation of the target mRNA is still inhibited. Mechanistically, this non-canonical regulation by sRNAs is poorly understood. Our previous work demonstrated repression of the mannose transporter manX mRNA by the sRNA SgrS, but the regulatory mechanism was unknown. Here, we report that manX translation is controlled by a molecular role-reversal mechanism where Hfq, not the sRNA, is the direct repressor. Hfq binding adjacent to the manX RBS is required for sRNA-mediated translational repression. Translation of manX is also regulated by another sRNA, DicF, via the same non-canonical Hfq-dependent mechanism. Our results suggest that the sRNAs recruit Hfq to its binding site or stabilize the mRNA-Hfq complex. This work adds to the growing number of examples of diverse mechanisms of translational regulation by sRNAs in bacteria.
机译:在细菌中,小RNA(sRNA)抑制翻译的典型机制涉及闭塞核糖体结合位点(RBS)的sRNA-mRNA碱基配对,直接阻止翻译。在这种机制中,sRNA是直接调控因子,而RNA伴侣Hfq通过稳定sRNA发挥辅助作用。有几个例子,其中sRNA并不直接干扰核糖体结合,但靶mRNA的翻译仍然受到抑制。从机理上讲,人们对sRNA的这种非经典调节知之甚少。我们以前的工作证明了sRNA SgrS对甘露糖转运蛋白manX mRNA的抑制作用,但调控机制尚不清楚。在这里,我们报道了manX翻译受分子作用逆转机制控制,其中Hfq(而不是sRNA)是直接阻遏物。 sRNA介导的翻译抑制需要与manX RBS相邻的Hfq结合。 manX的翻译也受另一个sRNA DicF的调节,它通过相同的非规范Hfq依赖性机制。我们的结果表明,sRNA将Hfq募集到其结合位点或稳定mRNA-Hfq复合物。这项工作增加了细菌中sRNA进行翻译调控的多种机制的例子。

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