| Literature DB >> 33766930 |
Jiahui Du1,2, Junjun Jing1, Shuo Chen1, Yuan Yuan1, Jifan Feng1, Thach-Vu Ho1, Prerna Sehgal1, Jian Xu1, Xinquan Jiang2, Yang Chai1.
Abstract
Stem cells self-renew or give rise to transit-amplifying cells (TACs) that differentiate into specific functional cell types. The fate determination of stem cells to TACs and their transition to fully differentiated progeny is precisely regulated to maintain tissue homeostasis. Arid1a, a core component of the switch/sucrose nonfermentable complex, performs epigenetic regulation of stage- and tissue-specific genes that is indispensable for stem cell homeostasis and differentiation. However, the functional mechanism of Arid1a in the fate commitment of mesenchymal stem cells (MSCs) and their progeny is not clear. Using the continuously growing adult mouse incisor model, we show that Arid1a maintains tissue homeostasis through limiting proliferation, promoting cell cycle exit and differentiation of TACs by inhibiting the Aurka-Cdk1 axis. Loss of Arid1a overactivates the Aurka-Cdk1 axis, leading to expansion of the mitotic TAC population but compromising their differentiation ability. Furthermore, the defective homeostasis after loss of Arid1a ultimately leads to reduction of the MSC population. These findings reveal the functional significance of Arid1a in regulating the fate of TACs and their interaction with MSCs to maintain tissue homeostasis.Entities:
Keywords: Arid1a; Cell cycle; Mesenchymal stem cells; Mitosis; Transit-amplifying cells
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Year: 2021 PMID: 33766930 PMCID: PMC8077510 DOI: 10.1242/dev.198838
Source DB: PubMed Journal: Development ISSN: 0950-1991 Impact factor: 6.868