The formation of HuR/YB1 complex is required for the stabilization of target mRNA to promote myogenesis

Author:

Sánchez Brenda Janice1234,Mubaid Souad34,Busque Sandrine34,de los Santos Yossef Lopez2,Ashour Kholoud34ORCID,Sadek Jason34,Lian Xian Jin34,Khattak Shahryar12,Di Marco Sergio1234,Gallouzi Imed-Eddine1234ORCID

Affiliation:

1. KAUST Smart-Health Initiative King Abdullah University of Science and Technology (KAUST) , Jeddah, Saudi Arabia

2. KAUST Biological Environmental Science and Engineering (BESE) Division, King Abdullah University of Science and Technology (KAUST) , Jeddah, Saudi Arabia

3. Dept. of Biochemistry, McGill University , 3655 Promenade Sir William Osler, Montreal, QC H3G1Y6, Canada

4. Rosalind & Morris Goodman Cancer Institute, McGill University , 1160 Pine Avenue, Montreal, QC H3A1A3, Canada

Abstract

AbstractmRNA stability is the mechanism by which cells protect transcripts allowing their expression to execute various functions that affect cell metabolism and fate. It is well-established that RNA binding proteins (RBPs) such as HuR use their ability to stabilize mRNA targets to modulate vital processes such as muscle fiber formation (myogenesis). However, the machinery and the mechanisms regulating mRNA stabilization are still elusive. Here, we identified Y-Box binding protein 1 (YB1) as an indispensable HuR binding partner for mRNA stabilization and promotion of myogenesis. Both HuR and YB1 bind to 409 common mRNA targets, 147 of which contain a U-rich consensus motif in their 3′ untranslated region (3′UTR) that can also be found in mRNA targets in other cell systems. YB1 and HuR form a heterodimer that associates with the U-rich consensus motif to stabilize key promyogenic mRNAs. The formation of this complex involves a small domain in HuR (227–234) that if mutated prevents HuR from reestablishing myogenesis in siHuR-treated muscle cells. Together our data uncover that YB1 is a key player in HuR-mediated stabilization of pro-myogenic mRNAs and provide the first indication that the mRNA stability mechanism is as complex as other key cellular processes such as mRNA decay and translation.

Funder

CIHR operating grant

CIHR project grant

Concejo Nacional de Ciencia y Tecnologia

Fonds de recherche du Québec—Nature et technologies

Charlotte and Leo Karrasik Graduate Studentship

Natural Sciences and Engineering Research Council of Canada

Taibah University-Ministry of Higher education

CIHR Studentship Award

Publisher

Oxford University Press (OUP)

Subject

Genetics

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