YB-1 unwinds mRNA secondary structures in vitro and negatively regulates stress granule assembly in HeLa cells

Author:

Budkina Karina12,El Hage Krystel1ORCID,Clément Marie-Jeanne1,Desforges Bénédicte1,Bouhss Ahmed1,Joshi Vandana1,Maucuer Alexandre1,Hamon Loic1ORCID,Ovchinnikov Lev P2,Lyabin Dmitry N2ORCID,Pastré David1ORCID

Affiliation:

1. SABNP, Univ Evry, INSERM U1204, Université Paris-Saclay, 91025 Evry, France

2. Institute of Protein Research, Russian Academy of Sciences, Pushchino, 142290, Russian Federation

Abstract

Abstract In the absence of the scanning ribosomes that unwind mRNA coding sequences and 5′UTRs, mRNAs are likely to form secondary structures and intermolecular bridges. Intermolecular base pairing of non polysomal mRNAs is involved in stress granule (SG) assembly when the pool of mRNAs freed from ribosomes increases during cellular stress. Here, we unravel the structural mechanisms by which a major partner of dormant mRNAs, YB-1 (YBX1), unwinds mRNA secondary structures without ATP consumption by using its conserved cold-shock domain to destabilize RNA stem/loops and its unstructured C-terminal domain to secure RNA unwinding. At endogenous levels, YB-1 facilitates SG disassembly during arsenite stress recovery. In addition, overexpression of wild-type YB-1 and to a lesser extent unwinding-defective mutants inhibit SG assembly in HeLa cells. Through its mRNA-unwinding activity, YB-1 may thus inhibit SG assembly in cancer cells and package dormant mRNA in an unfolded state, thus preparing mRNAs for translation initiation.

Funder

Région Ile-de-France

Russian Federation

Genopole

Marie Skłodowska-Curie

Inserm

Publisher

Oxford University Press (OUP)

Subject

Genetics

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