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首页> 外文期刊>MBio >The Leader Peptide peTrpL Forms Antibiotic-Containing Ribonucleoprotein Complexes for Posttranscriptional Regulation of Multiresistance Genes
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The Leader Peptide peTrpL Forms Antibiotic-Containing Ribonucleoprotein Complexes for Posttranscriptional Regulation of Multiresistance Genes

机译:领导肽PETRPL形成含抗生素的核糖蛋白复合物,用于对多术基因进行后扫描调节

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摘要

Bacterial ribosome-dependent attenuators are widespread posttranscriptional regulators. They harbor small upstream open reading frames (uORFs) encoding leader peptides, for which no functions in trans are known yet. In the plant symbiont Sinorhizobium meliloti , the tryptophan biosynthesis gene trpE(G) is preceded by the uORF trpL and is regulated by transcription attenuation according to tryptophan availability. However, trpLE(G) transcription is initiated independently of the tryptophan level in S. meliloti , thereby ensuring a largely tryptophan-independent production of the leader peptide peTrpL. Here, we provide evidence for a tryptophan-independent role of peTrpL in trans . We found that peTrpL increases the resistance toward tetracycline, erythromycin, chloramphenicol, and the flavonoid genistein, which are substrates of the major multidrug efflux pump SmeAB. Coimmunoprecipitation with a FLAG-peTrpL suggested smeR mRNA, which encodes the transcription repressor of smeABR , as a peptide target. Indeed, upon antibiotic exposure, smeR mRNA was destabilized and smeA stabilized in a peTrpL-dependent manner, showing that peTrpL acts in the differential regulation of smeABR . Furthermore, smeR mRNA was coimmunoprecipitated with peTrpL in antibiotic-dependent ribonucleoprotein (ARNP) complexes, which, in addition, contained an antibiotic-induced antisense RNA complementary to smeR . In vitro ARNP reconstitution revealed that the above-mentioned antibiotics and genistein directly support complex formation. A specific region of the antisense RNA was identified as a seed region for ARNP assembly in vitro . Altogether, our data show that peTrpL is involved in a mechanism for direct utilization of antimicrobial compounds in posttranscriptional regulation of multiresistance genes. Importantly, this role of peTrpL in resistance is conserved in other Alphaproteobacteria .
机译:细菌核糖体依赖性衰减器是广泛的后颅骨调节剂。它们涉及编码领导肽的小上游开放阅读框架(UORF),其中riss中没有任何功能。在植物symbiont sinorhizobium meliloti中,色氨酸生物合成基因Trpe(g)在UORF TrPL之前,根据色氨酸可用性通过转录衰减调节。然而,TRPLE(g)转录是独立于S.Meliloti的色氨酸水平启动的,从而确保了基本上是针对肽肽PETRPL的独立式非独立式生产。在这里,我们为跨境中的Trorplan独立作用提供了证据。我们发现PETRPL增加了对四环素,红霉素,氯霉素和类黄酮的抗性,这是主要多药中泵泵SMEAB的基板。与标志 - PETRPL建议的SMER mRNA的COIMMUNOPRECIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIPIAD,其编码SMEABR的转录阻遏物,作为肽靶标。实际上,在抗生素暴露时,SMER mRNA不稳定,以PETRPL依赖性方式稳定搅拌,表明PETRPL在SMEABR的差异调节中起作用。此外,SMER mRNA在抗生素依赖性核糖核糖蛋白(ARNP)复合物中用PETRPL与PETRPL共沉淀,其含有抗生素诱导的互补的SMER的反义RNA。体外arnp重构表明,上述抗生素和Genistein直接支持复杂的形成。体外鉴定反义RNA的特定区域作为ARNP组装的种子区域。完全,我们的数据表明,PETRPL涉及一种用于直接利用抗微生物化合物在多际基因的后剖析调节中的机制。重要的是,PETRPL在抵抗力中的这种作用在其他alphaproteobacteria中保守。

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