| Literature DB >> 28285904 |
Francisco M Barriga1, Elisa Montagni1, Miyeko Mana2, Maria Mendez-Lago3, Xavier Hernando-Momblona1, Marta Sevillano1, Amy Guillaumet-Adkins3, Gustavo Rodriguez-Esteban3, Simon J A Buczacki4, Marta Gut3, Holger Heyn3, Douglas J Winton4, Omer H Yilmaz2, Camille Stephan-Otto Attolini1, Ivo Gut3, Eduard Batlle5.
Abstract
Highly proliferative Lgr5+ stem cells maintain the intestinal epithelium and are thought to be largely homogeneous. Although quiescent intestinal stem cell (ISC) populations have been described, the identity and features of such a population remain controversial. Here we report unanticipated heterogeneity within the Lgr5+ ISC pool. We found that expression of the RNA-binding protein Mex3a labels a slowly cycling subpopulation of Lgr5+ ISCs that contribute to all intestinal lineages with distinct kinetics. Single-cell transcriptome profiling revealed that Lgr5+ cells adopt two discrete states, one of which is defined by a Mex3a expression program and relatively low levels of proliferation genes. During homeostasis, Mex3a+ cells continually shift into the rapidly dividing, self-renewing ISC pool. Chemotherapy and radiation preferentially target rapidly dividing Lgr5+ cells but spare the Mex3a-high/Lgr5+ population, helping to promote regeneration of the intestinal epithelium following toxic insults. Thus, Mex3a defines a reserve-like ISC population within the Lgr5+ compartment.Entities:
Keywords: Lgr5+ ISC heterogeneity; chemotherapy resistance; quiescent stem cell
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Year: 2017 PMID: 28285904 PMCID: PMC5774992 DOI: 10.1016/j.stem.2017.02.007
Source DB: PubMed Journal: Cell Stem Cell ISSN: 1875-9777 Impact factor: 24.633