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Publication : The Transcription Factor FOXN1 Regulates Skin Adipogenesis and Affects Susceptibility to Diet-Induced Obesity.

First Author  Walendzik K Year  2020
Journal  J Invest Dermatol Volume  140
Issue  6 Pages  1166-1175.e9
PubMed ID  31811821 Mgi Jnum  J:296918
Mgi Id  MGI:6441561 Doi  10.1016/j.jid.2019.11.010
Citation  Walendzik K, et al. (2020) The Transcription Factor FOXN1 Regulates Skin Adipogenesis and Affects Susceptibility to Diet-Induced Obesity. J Invest Dermatol 140(6):1166-1175.e9
abstractText  FOXN1, a transcription factor expressed in the epidermis, regulates keratinocyte differentiation and participates in skin wound healing. In this study, we explored the impact of FOXN1 insufficiency on diet-stimulated weight gain and dermal white adipose tissue regulation in the intact and wounded skin of FOXN1(eGFP/+) (heterozygotes, FOXN1-insufficient) mice in the context of age and diet. The results showed that on a high-fat diet, FOXN1(eGFP/+) mice gained significantly less body weight than their FOXN1(+/+) counterparts (FOXN1-sufficient mice). The intact and wounded skin of FOXN1(eGFP/+) mice displayed abrogated expression of the master regulators of adipogenesis, PPARgamma, FABP4, and leptin, which decreased with age in FOXN1(+/+) mice. FOXN1 insufficiency also resulted in a decreased percentage of adipocyte-committed precursor cells (CD24(+)) in the skin. The proadipogenic pathway genes Bmp2, Igf2, and Mest showed a gradual decrease in expression that accompanied the gradual inactivation of FOXN1 in the skin of FOXN1(+/+), FOXN1(eGFP/+), and FOXN1(eGFP/eGFP) (lack of FOXN1) mice. Bone morphogenetic protein 2 and insulin-like growth factor 2 signals colocalized with FOXN1-eGFP in the epidermis and in hair follicles. These data demonstrated that FOXN1 initiates the cascade of adipogenic signaling that regulates skin homeostasis and wound healing and affects susceptibility to diet-induced obesity.
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