4.8 Article

Non-canonical mechanism for translational control in bacteria: synthesis of ribosomal protein S1

Journal

EMBO JOURNAL
Volume 20, Issue 15, Pages 4222-4232

Publisher

WILEY
DOI: 10.1093/emboj/20.15.4222

Keywords

autogenous control; mRNA structure; phylogenetic analysis; ribosomal protein S1; translation initiation

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Translation initiation region (TIR) of the rpsA mRNA encoding ribosomal protein S1 is one of the most efficient in Escherichia coli despite the absence of a canonical Shine-Dalgarno-element. Its high efficiency is under strong negative autogenous control, a puzzling phenomenon as S1 has no strict sequence specificity. To define sequence and structural elements responsible for translational efficiency and autoregulation of the rpsA mRNA, a series of rpsA'-'lac Z chromosomal fusions bearing various mutations in the rpsA TIR was created and tested for beta -galactosidase activity in the absence and presence of excess S1. These in vivo results, as well as data obtained by in vitro techniques and phylogenetic comparison, allow us to propose a model for the structural and functional organization of the rpsA TIR specific for proteobacteria related to E.coli. According to the model, the high efficiency of translation initiation is provided by a specific fold of the rpsA leader forming a non-contiguous ribosome entry site, which is destroyed upon binding of free SI when it acts as an autogenous repressor.

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