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Publication : An evolutionarily conserved ribosome-rescue pathway maintains epidermal homeostasis.

First Author  Liakath-Ali K Year  2018
Journal  Nature Volume  556
Issue  7701 Pages  376-380
PubMed ID  29643507 Mgi Jnum  J:261638
Mgi Id  MGI:6155782 Doi  10.1038/s41586-018-0032-3
Citation  Liakath-Ali K, et al. (2018) An evolutionarily conserved ribosome-rescue pathway maintains epidermal homeostasis. Nature 556(7701):376-380
abstractText  Ribosome-associated mRNA quality control mechanisms ensure the fidelity of protein translation(1,2). Although these mechanisms have been extensively studied in yeast, little is known about their role in mammalian tissues, despite emerging evidence that stem cell fate is controlled by translational mechanisms(3,4). One evolutionarily conserved component of the quality control machinery, Dom34 (in higher eukaryotes known as Pelota (Pelo)), rescues stalled ribosomes (5) . Here we show that Pelo is required for mammalian epidermal homeostasis. Conditional deletion of Pelo in mouse epidermal stem cells that express Lrig1 results in hyperproliferation and abnormal differentiation of these cells. By contrast, deletion of Pelo in Lgr5-expressing stem cells has no effect and deletion in Lgr6-expressing stem cells induces only a mild phenotype. Loss of Pelo results in accumulation of short ribosome footprints and global upregulation of translation, rather than affecting the expression of specific genes. Translational inhibition by rapamycin-mediated downregulation of mTOR (mechanistic target of rapamycin kinase) rescues the epidermal phenotype. Our study reveals that the ribosome-rescue machinery is important for mammalian tissue homeostasis and that it has specific effects on different stem cell populations.
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