| Literature DB >> 34875230 |
Kasun Buddika1, Yi-Ting Huang1, Ishara S Ariyapala1, Alex Butrum-Griffith1, Sam A Norrell1, Alex M O'Connor1, Viraj K Patel1, Samuel A Rector1, Mark Slovan1, Mallory Sokolowski1, Yasuko Kato2, Akira Nakamura3, Nicholas S Sokol4.
Abstract
The role of processing bodies (P-bodies), key sites of post-transcriptional control, in adult stem cells remains poorly understood. Here, we report that adult Drosophila intestinal stem cells, but not surrounding differentiated cells such as absorptive enterocytes (ECs), harbor P-bodies that contain Drosophila orthologs of mammalian P-body components DDX6, EDC3, EDC4, and LSM14A/B. A targeted RNAi screen in intestinal progenitor cells identified 39 previously known and 64 novel P-body regulators, including Patr-1, a gene necessary for P-body assembly. Loss of Patr-1-dependent P-bodies leads to a loss of stem cells that is associated with inappropriate expression of EC-fate gene nubbin. Transcriptomic analysis of progenitor cells identifies a cadre of such weakly transcribed pro-differentiation transcripts that are elevated after P-body loss. Altogether, this study identifies a P-body-dependent repression activity that coordinates with known transcriptional repression programs to maintain a population of in vivo stem cells in a state primed for differentiation. Published by Elsevier Inc.Entities:
Keywords: FMRP; ISCs; Me31B; P-bodies; Patr-1; TRAL; intestinal stem cells; stress granules
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Year: 2021 PMID: 34875230 PMCID: PMC8792327 DOI: 10.1016/j.cub.2021.11.032
Source DB: PubMed Journal: Curr Biol ISSN: 0960-9822 Impact factor: 10.834