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Genome-Wide Effects of Selenium and Translational Uncoupling on Transcription in the Termite Gut Symbiont Treponema primitia

机译:硒和翻译解偶联对白蚁肠道共生菌梅毒螺旋体初发中转录的全基因组影响

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When prokaryotic cells acquire mutations, encounter translation-inhibiting substances, or experience adverse environmental conditions that limit their ability to synthesize proteins, transcription can become uncoupled from translation. Such uncoupling is known to suppress transcription of protein-encoding genes in bacteria. Here we show that the trace element selenium controls transcription of the gene for the selenocysteine-utilizing enzyme formate dehydrogenase (fdhFSec) through a translation-coupled mechanism in the termite gut symbiont Treponema primitia, a member of the bacterial phylum Spirochaetes. We also evaluated changes in genome-wide transcriptional patterns caused by selenium limitation and by generally uncoupling translation from transcription via antibiotic-mediated inhibition of protein synthesis. We observed that inhibiting protein synthesis in T.?primitia influences transcriptional patterns in unexpected ways. In addition to suppressing transcription of certain genes, the expected consequence of inhibiting protein synthesis, we found numerous examples in which transcription of genes and operons is truncated far downstream from putative promoters, is unchanged, or is even stimulated overall. These results indicate that gene regulation in bacteria allows for specific post-initiation transcriptional responses during periods of limited protein synthesis, which may depend both on translational coupling and on unclassified intrinsic elements of protein-encoding genes. >IMPORTANCE A large body of literature demonstrates that the coupling of transcription and translation is a general and essential method by which bacteria regulate gene expression levels. However, the potential role of noncanonical amino acids in regulating transcriptional output via translational control remains, for the most part, undefined. Furthermore, the genome-wide transcriptional state in response to translational decoupling is not well quantified. The results presented here suggest that the noncanonical amino acid selenocysteine is able to tune transcription of an important metabolic gene via translational coupling. Furthermore, a genome-wide analysis reveals that transcriptional decoupling produces a wide-ranging effect and that this effect is not uniform. These results exemplify how growth conditions that impact translational processivity can rapidly feed back on transcriptional productivity of prespecified groups of genes, providing bacteria with an efficient response to environmental changes.
机译:当原核细胞发生突变,遇到翻译抑制物质或遇到不利的环境条件(这些条件限制了它们合成蛋白质的能力)时,转录可能会与翻译脱钩。已知这种解偶联可抑制细菌中蛋白质编码基因的转录。在这里,我们显示了微量元素硒通过白蚁肠道共生体中的翻译偶联机制控制硒代半胱氨酸利用酶甲酸脱氢酶( fdhF Sec )基因的转录 Treponema primitia ,细菌门 Spirochaetes 的成员。我们还评估了硒限制和一般通过抗生素介导的蛋白质合成抑制使转录与转录脱钩而引起的全基因组转录模式的变化。我们观察到抑制 T.?primitia 中的蛋白质合成会以意想不到的方式影响转录模式。除了抑制某些基因的转录,抑制蛋白质合成的预期结果外,我们还发现了许多例子,其中基因和操纵子的转录在推定的启动子下游被截短,没有改变,甚至整体上受到刺激。这些结果表明,细菌的基因调控可在有限的蛋白质合成期间实现特定的起始后转录反应,这可能既取决于翻译偶联,又取决于蛋白质编码基因的未分类内在因素。 >重要性大量文献表明,转录和翻译的结合是细菌调节基因表达水平的通用且必不可少的方法。然而,在大多数情况下,非典型氨基酸在通过翻译控制调节转录输出中的潜在作用仍然不确定。此外,响应翻译解耦的全基因组转录状态不能很好地量化。此处显示的结果表明,非经典氨基酸硒代半胱氨酸能够通过翻译偶联调节重要的代谢基因的转录。此外,全基因组分析揭示了转录解偶联产生了广泛的作用,并且这种作用是不均匀的。这些结果说明了影响翻译过程的生长条件如何快速反馈预定基因组的转录生产力,从而为细菌提供了对环境变化的有效响应。

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