A stem cell roadmap of ribosome heterogeneity reveals a function for RPL10A in mesoderm production

Author:

Genuth Naomi R.ORCID,Shi Zhen,Kunimoto Koshi,Hung VictoriaORCID,Xu Adele F.ORCID,Kerr Craig H.,Tiu Gerald C.,Oses-Prieto Juan A.ORCID,Salomon-Shulman Rachel E. A.,Axelrod Jeffrey D.ORCID,Burlingame Alma L.ORCID,Loh Kyle M.ORCID,Barna MariaORCID

Abstract

AbstractRecent findings suggest that the ribosome itself modulates gene expression. However, whether ribosomes change composition across cell types or control cell fate remains unknown. Here, employing quantitative mass spectrometry during human embryonic stem cell differentiation, we identify dozens of ribosome composition changes underlying cell fate specification. We observe upregulation of RPL10A/uL1-containing ribosomes in the primitive streak followed by progressive decreases during mesoderm differentiation. An Rpl10a loss-of-function allele in mice causes striking early mesodermal phenotypes, including posterior trunk truncations, and inhibits paraxial mesoderm production in culture. Ribosome profiling in Rpl10a loss-of-function mice reveals decreased translation of mesoderm regulators, including Wnt pathway mRNAs, which are also enriched on RPL10A/uL1-containing ribosomes. We further show that RPL10A/uL1 regulates canonical and non-canonical Wnt signaling during stem cell differentiation and in the developing embryo. These findings reveal unexpected ribosome composition modularity that controls differentiation and development through the specialized translation of key signaling networks.

Funder

New York Stem Cell Foundation

U.S. Department of Health & Human Services | National Institutes of Health

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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