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Hildebrandt, Andrea; Brüggemann, Mirko; Rücklé, Cornelia; Boerner, Susan; Heidelberger, Jan B; Busch, Anke; Hänel, Heike; Voigt, Andrea; Möckel, Martin M; Ebersberger, Stefanie; Scholz, Anica; Dold, Annabelle; Schmid, Tobias; Ebersberger, Ingo; Roignant, Jean-Yves; Zarnack, Kathi; König, Julian; Beli, Petra
Genome Biology, 10/2019, Letnik: 20, Številka: 1Journal Article
Cells have evolved quality control mechanisms to ensure protein homeostasis by detecting and degrading aberrant mRNAs and proteins. A common source of aberrant mRNAs is premature polyadenylation, which can result in non-functional protein products. Translating ribosomes that encounter poly(A) sequences are terminally stalled, followed by ribosome recycling and decay of the truncated nascent polypeptide via ribosome-associated quality control. Here, we demonstrate that the conserved RNA-binding E3 ubiquitin ligase Makorin Ring Finger Protein 1 (MKRN1) promotes ribosome stalling at poly(A) sequences during ribosome-associated quality control. We show that MKRN1 directly binds to the cytoplasmic poly(A)-binding protein (PABPC1) and associates with polysomes. MKRN1 is positioned upstream of poly(A) tails in mRNAs in a PABPC1-dependent manner. Ubiquitin remnant profiling and in vitro ubiquitylation assays uncover PABPC1 and ribosomal protein RPS10 as direct ubiquitylation substrates of MKRN1. We propose that MKRN1 mediates the recognition of poly(A) tails to prevent the production of erroneous proteins from prematurely polyadenylated transcripts, thereby maintaining proteome integrity.
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