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Structural Dynamics of the YidC:Ribosome Complex during Membrane Protein Biogenesis.


ABSTRACT: Members of the YidC/Oxa1/Alb3 family universally facilitate membrane protein biogenesis, via mechanisms that have thus far remained unclear. Here, we investigated two crucial functional aspects: the interaction of YidC with ribosome:nascent chain complexes (RNCs) and the structural dynamics of RNC-bound YidC in nanodiscs. We observed that a fully exposed nascent transmembrane domain (TMD) is required for high-affinity YidC:RNC interactions, while weaker binding may already occur at earlier stages of translation. YidC efficiently catalyzed the membrane insertion of nascent TMDs in both fluid and gel phase membranes. Cryo-electron microscopy and fluorescence analysis revealed a conformational change in YidC upon nascent chain insertion: the essential TMDs 2 and 3 of YidC were tilted, while the amphipathic helix EH1 relocated into the hydrophobic core of the membrane. We suggest that EH1 serves as a mechanical lever, facilitating a coordinated movement of YidC TMDs to trigger the release of nascent chains into the membrane.

SUBMITTER: Kedrov A 

PROVIDER: S-EPMC5186731 | biostudies-literature | 2016 Dec

REPOSITORIES: biostudies-literature

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Structural Dynamics of the YidC:Ribosome Complex during Membrane Protein Biogenesis.

Kedrov Alexej A   Wickles Stephan S   Crevenna Alvaro H AH   van der Sluis Eli O EO   Buschauer Robert R   Berninghausen Otto O   Lamb Don C DC   Beckmann Roland R  

Cell reports 20161201 11


Members of the YidC/Oxa1/Alb3 family universally facilitate membrane protein biogenesis, via mechanisms that have thus far remained unclear. Here, we investigated two crucial functional aspects: the interaction of YidC with ribosome:nascent chain complexes (RNCs) and the structural dynamics of RNC-bound YidC in nanodiscs. We observed that a fully exposed nascent transmembrane domain (TMD) is required for high-affinity YidC:RNC interactions, while weaker binding may already occur at earlier stage  ...[more]

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