| Literature DB >> 30765604 |
An-Qi Li1, Zhan-Peng Sun1, Xu Liu1, Jin-Shu Yang1, Feng Jin1, Lin Zhu1, Wen-Huan Jia1, Stephanie De Vos2, Gilbert Van Stappen2, Peter Bossier2, Wei-Jun Yang3,4.
Abstract
Cellular quiescence, a reversible state in which growth, proliferation, and other cellular activities are arrested, is important for self-renewal, differentiation, development, regeneration, and stress resistance. However, the physiological mechanisms underlying cellular quiescence remain largely unknown. In the present study, we used embryos of the crustacean Artemia in the diapause stage, in which these embryos remain quiescent for prolonged periods, as a model to explore the relationship between cell-membrane potential (V mem) and quiescence. We found that V mem is hyperpolarized and that the intracellular chloride concentration is high in diapause embryos, whereas V mem is depolarized and intracellular chloride concentration is reduced in postdiapause embryos and during further embryonic development. We identified and characterized the chloride ion channel protein cystic fibrosis transmembrane conductance regulator (CFTR) of Artemia (Ar-CFTR) and found that its expression is silenced in quiescent cells of Artemia diapause embryos but remains constant in all other embryonic stages. Ar-CFTR knockdown and GlyH-101-mediated chemical inhibition of Ar-CFTR produced diapause embryos having a high V mem and intracellular chloride concentration, whereas control Artemia embryos released free-swimming nauplius larvae. Transcriptome analysis of embryos at different developmental stages revealed that proliferation, differentiation, and metabolism are suppressed in diapause embryos and restored in postdiapause embryos. Combined with RNA sequencing (RNA-Seq) of GlyH-101-treated MCF-7 breast cancer cells, these analyses revealed that CFTR inhibition down-regulates the Wnt and Aurora Kinase A (AURKA) signaling pathways and up-regulates the p53 signaling pathway. Our findings provide insight into CFTR-mediated regulation of cellular quiescence and V mem in the Artemia model.Entities:
Keywords: Artemia; cell cycle; cell proliferation; cellular quiescence; channel activation; chloride channel; cystic fibrosis transmembrane conductance regulator (CFTR); diapause embryo; dormancy maintenance; hyperpolarization
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Year: 2019 PMID: 30765604 PMCID: PMC6484108 DOI: 10.1074/jbc.RA118.005900
Source DB: PubMed Journal: J Biol Chem ISSN: 0021-9258 Impact factor: 5.157