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Publication : Embryogenic stem cell-derived intestinal crypt fission directs de novo crypt genesis.

First Author  Huang XT Year  2022
Journal  Cell Rep Volume  41
Issue  11 Pages  111796
PubMed ID  36516755 Mgi Jnum  J:332247
Mgi Id  MGI:7413794 Doi  10.1016/j.celrep.2022.111796
Citation  Huang XT, et al. (2022) Embryogenic stem cell-derived intestinal crypt fission directs de novo crypt genesis. Cell Rep 41(11):111796
abstractText  Intestinal epithelial replenishment is fueled by continuously dividing intestinal stem cells (ISCs) resident at the crypt niche. However, the cell type(s) enabling replenishment upon damage and subsequent loss of whole crypts remain largely unclear. Using Set domain-containing protein 4 (Setd4), we identify a small population with reserve stem cell characteristics in the mouse intestine. Upon irradiation-induced injury, Setd4-expressing (Setd4(+)) cells survive radiation exposure and then activate to produce Sca-1-expressing cell types to restore the epithelial wall and regenerate crypts de novo via crypt fission. Setd4(+) cells are confirmed to originate from the early fetal period, subsequently contributing to the development of embryonic gut and the establishment of postnatal crypts. Setd4(+) cells are therefore represented as both originators and key regenerators of the intestine.
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