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Publication : aPKCĪ» controls epidermal homeostasis and stem cell fate through regulation of division orientation.

First Author  Niessen MT Year  2013
Journal  J Cell Biol Volume  202
Issue  6 Pages  887-900
PubMed ID  24019538 Mgi Jnum  J:201737
Mgi Id  MGI:5515649 Doi  10.1083/jcb.201307001
Citation  Niessen MT, et al. (2013) aPKClambda controls epidermal homeostasis and stem cell fate through regulation of division orientation. J Cell Biol 202(6):887-900
abstractText  The atypical protein kinase C (aPKC) is a key regulator of polarity and cell fate in lower organisms. However, whether mammalian aPKCs control stem cells and fate in vivo is not known. Here we show that loss of aPKClambda in a self-renewing epithelium, the epidermis, disturbed tissue homeostasis, differentiation, and stem cell dynamics, causing progressive changes in this tissue. This was accompanied by a gradual loss of quiescent hair follicle bulge stem cells and a temporary increase in proliferating progenitors. Lineage tracing analysis showed that loss of aPKClambda altered the fate of lower bulge/hair germ stem cells. This ultimately led to loss of proliferative potential, stem cell exhaustion, alopecia, and premature aging. Inactivation of aPKClambda produced more asymmetric divisions in different compartments, including the bulge. Thus, aPKClambda is crucial for homeostasis of self-renewing stratifying epithelia, and for the regulation of cell fate, differentiation, and maintenance of epidermal bulge stem cells likely through its role in balancing symmetric and asymmetric division.
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