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首页> 外文期刊>Nucleic Acids Research >RppH-dependent pyrophosphohydrolysis of mRNAs is regulated by direct interaction with DapF in Escherichia coli
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RppH-dependent pyrophosphohydrolysis of mRNAs is regulated by direct interaction with DapF in Escherichia coli

机译:RppH依赖性的mRNA的焦磷酸水解是通过与DapF在大肠杆菌中的直接相互作用来调节的。

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摘要

Similar to decapping of eukaryotic mRNAs, the RppH-catalyzed conversion of 5'-terminal triphosphate to monophosphate has recently been identified as the rate-limiting step for the degradation of a subset of mRNAs in Escherichia coli. However, the regulation of RppH pyrophosphohydrolase activity is not well understood. Because the overexpression of RppH alone does not affect the decay rate of most target mRNAs, the existence of a mechanism regulating its activity has been suggested. In this study, we identified DapF, a diaminopimelate (DAP) epimerase catalyzing the stereoinversion of L,L-DAP to meso-DAP, as a regulator of RppH. DapF showed a high affinity interaction with RppH and increased its RNA pyrophosphohydrolase activity. The simultaneous overexpression of both DapF and RppH increased the decay rates of RppH target RNAs by about a factor of two. Together, our data suggest that the cellular level of DapF is a critical factor regulating the RppH-catalyzed pyrophosphate removal and the subsequent degradation of target mRNAs.
机译:类似于真核mRNA的脱盖,最近已确定RppH催化的5'-末端三磷酸酯转化为单磷酸酯是大肠杆菌中mRNA子集降解的限速步骤。但是,RppH焦磷酸水解酶活性的调节尚不十分清楚。因为单独的RppH的过表达不会影响大多数目标mRNA的衰减率,所以建议存在调节其活性的机制。在这项研究中,我们确定DapF,一种二氨基庚二酸酯(DAP)差向异构酶,催化L,L-DAP立体转化为meso-DAP,是RppH的调节剂。 DapF显示与RppH的高亲和力相互作用,并增加其RNA焦磷酸水解酶的活性。 DapF和RppH的同时过表达使RppH靶RNA的衰变速率增加了大约两倍。在一起,我们的数据表明DapF的细胞水平是调节RppH催化焦磷酸盐去除和随后的目标mRNA降解的关键因素。

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