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Molecular basis of mRNA delivery to the bacterial ribosome.


ABSTRACT: Protein synthesis begins with the formation of a ribosome-mRNA complex. In bacteria, the 30S ribosomal subunit is recruited to many mRNAs through base pairing with the Shine Dalgarno (SD) sequence and RNA binding by ribosomal protein bS1. Translation can initiate on nascent mRNAs and RNA polymerase (RNAP) can promote recruitment of the pioneering 30S subunit. Here we examined ribosome recruitment to nascent mRNAs using cryo-EM, single-molecule fluorescence co-localization, and in-cell crosslinking mass spectrometry. We show that bS1 delivers the mRNA to the ribosome for SD duplex formation and 30S subunit activation. Additionally, bS1 mediates the stimulation of translation initiation by RNAP. Together, our work provides a mechanistic framework for how the SD duplex, ribosomal proteins and RNAP cooperate in 30S recruitment to mRNAs and establish transcription-translation coupling.

SUBMITTER: Webster MW 

PROVIDER: S-EPMC10983998 | biostudies-literature | 2024 Mar

REPOSITORIES: biostudies-literature

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Molecular basis of mRNA delivery to the bacterial ribosome.

Webster Michael W MW   Chauvier Adrien A   Rahil Huma H   Graziadei Andrea A   Charles Kristine K   Takacs Maria M   Saint-André Charlotte C   Rappsilber Juri J   Walter Nils G NG   Weixlbaumer Albert A  

bioRxiv : the preprint server for biology 20240319


Protein synthesis begins with the formation of a ribosome-mRNA complex. In bacteria, the 30S ribosomal subunit is recruited to many mRNAs through base pairing with the Shine Dalgarno (SD) sequence and RNA binding by ribosomal protein bS1. Translation can initiate on nascent mRNAs and RNA polymerase (RNAP) can promote recruitment of the pioneering 30S subunit. Here we examined ribosome recruitment to nascent mRNAs using cryo-EM, single-molecule fluorescence co-localization, and in-cell crosslinki  ...[more]

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