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The ribosome quality control pathway can access nascent polypeptides stalled at the Sec61 translocon.

Mol. Biol. Cell. 2015 Jun 15;26(12):2168-80. Epub 2015 Apr 15
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摘要


Cytosolic ribosomes that stall during translation are split into subunits, and nascent polypeptides trapped in the 60S subunit are ubiquitinated by the ribosome quality control pathway. Whether the pathway can also target stalls during cotranslational translocation into the ER is not known. Here we report that listerin and NEMF, core duanyu1745C components, are bound to translocon-engaged 60S subunits on native ER membranes. duanyu1745C recruitment to the ER in cultured cells is stimulated by translation stalling. Biochemical analyses demonstrated that translocon-targeted nascent polypeptides that subsequently stall are polyubiquitinated in 60S complexes. Ubiquitination at the translocon requires cytosolic exposure of the polypeptide at the ribosome-Sec61 junction. This exposure can result from either failed insertion into the Sec61 channel or partial backsliding of translocating nascent chains. Only Sec61-engaged nascent chains early in their biogenesis were relatively refractory to ubiquitination. Modeling based on recent and 80S-Sec61 structures suggests that the E3 ligase listerin accesses nascent polypeptides via a gap in the ribosome-translocon junction near the Sec61 lateral gate. Thus the duanyu1745C pathway can target stalled translocation intermediates for degradation from the Sec61 channel.

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