Literature DB >> 33318147

Satellite cell expansion is mediated by P-eIF2α-dependent Tacc3 translation.

Ryo Fujita1,2, Solène Jamet2, Graham Lean1,2, Harry Chun Man Cheng1,2, Steven Hébert2, Claudia L Kleinman1,2, Colin Crist3,2.   

Abstract

Translational control of gene expression is an important regulator of adult stem cell quiescence, activation and self-renewal. In skeletal muscle, quiescent satellite cells maintain low levels of protein synthesis, mediated in part through the phosphorylation of eIF2α (P-eIF2α). Pharmacological inhibition of the eIF2α phosphatase with the small molecule sal003 maintains P-eIF2α and permits the expansion of satellite cells ex vivo Paradoxically, P-eIF2α also increases the translation of specific mRNAs, which is mediated by P-eIF2α-dependent read-through of inhibitory upstream open reading frames (uORFs). Here, we ask whether P-eIF2α-dependent mRNA translation enables expansion of satellite cells. Using transcriptomic and proteomic analyses, we show a number of genes associated with the assembly of the spindle pole to be upregulated at the level of protein, without corresponding change in mRNA levels, in satellite cells expanded in the presence of sal003. We show that uORFs in the 5' UTR of mRNA for the mitotic spindle stability gene Tacc3 direct P-eIF2α-dependent translation. Satellite cells deficient for TACC3 exhibit defects in expansion, self-renewal and regeneration of skeletal muscle.
© 2021. Published by The Company of Biologists Ltd.

Entities:  

Keywords:  Muscle stem cell; Satellite cell; Skeletal muscle regeneration; TACC3

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Year:  2021        PMID: 33318147     DOI: 10.1242/dev.194480

Source DB:  PubMed          Journal:  Development        ISSN: 0950-1991            Impact factor:   6.862


  3 in total

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