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Molecular basis of binding between the global post-transcriptional regulator CsrA and the T3SS chaperone CesT.


ABSTRACT: The T3SS chaperone CesT is recently shown to interact with the post-transcriptional regulator CsrA to modulate post-attachment signaling in enteropathogenic and enterohemorrhagic Escherichia coli. The molecular basis of the CesT/CsrA binding, however, remains elusive. Here, we show that CesT and CsrA both created two ligand binding sites in their homodimers, forming irregular multimeric complexes in solution. Through construction of a recombinant CsrA-dimer (Re-CsrA) that contains a single CesT binding site, the atomic binding features between CesT and CsrA are delineated via the structure of the CesT/Re-CsrA complex. In contrast to a previously reported N-terminally swapped dimer-form, CesT adopts a dimeric architecture with a swapped C-terminal helix for CsrA engagement. In CsrA, CesT binds to a surface patch that extensively overlaps with its mRNA binding site. The binding mode therefore justifies a mechanism of CsrA-modulation by CesT via competitive inhibition of the CsrA/mRNA interactions.

SUBMITTER: Ye F 

PROVIDER: S-EPMC5864733 | biostudies-literature | 2018 Mar

REPOSITORIES: biostudies-literature

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Molecular basis of binding between the global post-transcriptional regulator CsrA and the T3SS chaperone CesT.

Ye Fei F   Yang Fanli F   Yu Ruijie R   Lin Xi X   Qi Jianxun J   Chen Zhujun Z   Cao Yu Y   Wei Yuquan Y   Gao George F GF   Lu Guangwen G  

Nature communications 20180322 1


The T3SS chaperone CesT is recently shown to interact with the post-transcriptional regulator CsrA to modulate post-attachment signaling in enteropathogenic and enterohemorrhagic Escherichia coli. The molecular basis of the CesT/CsrA binding, however, remains elusive. Here, we show that CesT and CsrA both created two ligand binding sites in their homodimers, forming irregular multimeric complexes in solution. Through construction of a recombinant CsrA-dimer (Re-CsrA) that contains a single CesT  ...[more]

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