| Literature DB >> 30773316 |
Rastislav Horos1, Magdalena Büscher2, Rozemarijn Kleinendorst2, Anne-Marie Alleaume2, Abul K Tarafder2, Thomas Schwarzl2, Dmytro Dziuba2, Christian Tischer2, Elisabeth M Zielonka2, Asli Adak2, Alfredo Castello3, Wolfgang Huber2, Carsten Sachse4, Matthias W Hentze5.
Abstract
Vault RNAs (vtRNA) are small non-coding RNAs transcribed by RNA polymerase III found in many eukaryotes. Although they have been linked to drug resistance, apoptosis, and viral replication, their molecular functions remain unclear. Here, we show that vault RNAs directly bind the autophagy receptor sequestosome-1/p62 in human and murine cells. Overexpression of human vtRNA1-1 inhibits, while its antisense LNA-mediated knockdown enhances p62-dependent autophagy. Starvation of cells reduces the steady-state and p62-bound levels of vault RNA1-1 and induces autophagy. Mechanistically, p62 mutants that fail to bind vtRNAs display increased p62 homo-oligomerization and augmented interaction with autophagic effectors. Thus, vtRNA1-1 directly regulates selective autophagy by binding p62 and interference with oligomerization, a critical step of p62 function. Our data uncover a striking example of the potential of RNA to control protein functions directly, as previously recognized for protein-protein interactions and post-translational modifications.Entities:
Keywords: SQSTM1; autophagy; non-coding RNA; p62; sequestosome-1; starvation; vault RNA; vtRNA; vtRNA1-1
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Year: 2019 PMID: 30773316 DOI: 10.1016/j.cell.2019.01.030
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582