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Article Abstract

The emerging human enteropathogen is the main cause of diarrhea associated with antibiotherapy. Regulatory pathways underlying the adaptive responses remain understudied and the global view of promoter structure is still missing. In the genome of 630, 22 genes encoding sigma factors are present suggesting a complex pattern of transcription in this bacterium. We present here the first transcriptional map of the genome resulting from the identification of transcriptional start sites (TSS), promoter motifs and operon structures. By 5'-end RNA-seq approach, we mapped more than 1000 TSS upstream of genes. In addition to these primary TSS, this analysis revealed complex structure of transcriptional units such as alternative and internal promoters, potential RNA processing events and 5' untranslated regions. By following an iterative strategy that used as an input previously published consensus sequences and transcriptomic analysis, we identified candidate promoters upstream of most of protein-coding and non-coding RNAs genes. This strategy also led to refine consensus sequences of promoters recognized by major sigma factors of . Detailed analysis focuses on the transcription in the pathogenicity locus and regulatory genes, as well as regulons of transition phase and sporulation sigma factors as important components of regulatory network governing toxin gene expression and spore formation. Among the still uncharacterized regulons of the major sigma factors of , we defined the SigL regulon by combining transcriptome and analyses. We showed that the SigL regulon is largely involved in amino-acid degradation, a metabolism crucial for gut colonization. Finally, we combined our TSS mapping, identification of promoters and RNA-seq data to improve gene annotation and to suggest operon organization in . These data will considerably improve our knowledge of global regulatory circuits controlling gene expression in and will serve as a useful rich resource for scientific community both for the detailed analysis of specific genes and systems biology studies.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7438776PMC
http://dx.doi.org/10.3389/fmicb.2020.01939DOI Listing

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