Long non-coding RNA Neat1 and paraspeckle components are translational regulators in hypoxia

Author:

Godet Anne-Claire1,Roussel Emilie1,David Florian1ORCID,Hantelys Fransky1,Morfoisse Florent1,Alves Joffrey1,Pujol Françoise1,Ader Isabelle2,Bertrand Edouard3,Burlet-Schiltz Odile4,Froment Carine4ORCID,Henras Anthony K5,Vitali Patrice5,Lacazette Eric1,Tatin Florence1,Garmy-Susini Barbara1,Prats Anne-Catherine1ORCID

Affiliation:

1. UMR 1297-I2MC, Inserm, Université de Toulouse

2. UMR 1301-RESTORE, Inserm, CNRS 5070, Etablissement Français du Sang-Occitanie (EFS), National Veterinary School of Toulouse (ENVT), Université de Toulouse

3. UMR5535 CNRS-IGMM, Université de Montpellier

4. Institut de Pharmacologie et Biologie Structurale (IPBS), Université de Toulouse, CNRS

5. Molecular, Cellular and Developmental Biology Unit (MCD), Centre de Biologie Intégrative (CBI), Université de Toulouse

Abstract

Internal ribosome entry sites (IRESs) drive translation initiation during stress. In response to hypoxia, (lymph)angiogenic factors responsible for tissue revascularization in ischemic diseases are induced by the IRES-dependent mechanism. Here, we searched for IRES trans-acting factors (ITAFs) active in early hypoxia in mouse cardiomyocytes. Using knock-down and proteomics approaches, we show a link between a stressed-induced nuclear body, the paraspeckle, and IRES-dependent translation. Furthermore, smiFISH experiments demonstrate the recruitment of IRES-containing mRNA into paraspeckle during hypoxia. Our data reveal that the long non-coding RNA Neat1, an essential paraspeckle component, is a key translational regulator, active on IRESs of (lymph)angiogenic and cardioprotective factor mRNAs. In addition, paraspeckle proteins p54nrb and PSPC1 as well as nucleolin and RPS2, two p54nrb-interacting proteins identified by mass spectrometry, are ITAFs for IRES subgroups. Paraspeckle thus appears as a platform to recruit IRES-containing mRNAs and possibly host IRESome assembly. Polysome PCR array shows that Neat1 isoforms regulate IRES-dependent translation and, more widely, translation of mRNAs involved in stress response.

Funder

Agence Nationale de la Recherche

Ligue Contre le Cancer

Publisher

eLife Sciences Publications, Ltd

Subject

General Immunology and Microbiology,General Biochemistry, Genetics and Molecular Biology,General Medicine,General Neuroscience

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