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Artikel ; Online: Epiregulin as an Alternative Ligand for Leptin Receptor Alleviates Glucose Intolerance without Change in Obesity

No-Joon Song / Aejin Lee / Rumana Yasmeen / Qiwen Shen / Kefeng Yang / Shashi Bhushan Kumar / Danah Muhanna / Shanvanth Arnipalli / Sabrena F. Noria / Bradley J. Needleman / Jeffrey W. Hazey / Dean J. Mikami / Joana Ortega-Anaya / Rafael Jiménez-Flores / Jeremy Prokop / Ouliana Ziouzenkova

Cells, Vol 11, Iss 425, p

2022  Band 425

Abstract: The leptin receptor (LepR) acts as a signaling nexus for the regulation of glucose uptake and obesity, among other metabolic responses. The functional role of LepR under leptin-deficient conditions remains unclear. This study reports that epiregulin ( ... ...

Abstract The leptin receptor (LepR) acts as a signaling nexus for the regulation of glucose uptake and obesity, among other metabolic responses. The functional role of LepR under leptin-deficient conditions remains unclear. This study reports that epiregulin (EREG) governed glucose uptake in vitro and in vivo in Lep ob mice by activating LepR under leptin-deficient conditions. Single and long-term treatment with EREG effectively rescued glucose intolerance in comparative insulin and EREG tolerance tests in Lep ob mice. The immunoprecipitation study revealed binding between EREG and LepR in adipose tissue of Lep ob mice. EREG/LepR regulated glucose uptake without changes in obesity in Lep ob mice via mechanisms, including ERK activation and translocation of GLUT4 to the cell surface. EREG-dependent glucose uptake was abolished in Lepr db mice which supports a key role of LepR in this process. In contrast, inhibition of the canonical epidermal growth factor receptor (EGFR) pathway implicated in other EREG responses, increased glucose uptake. Our data provide a basis for understanding glycemic responses of EREG that are dependent on LepR unlike functions mediated by EGFR, including leptin secretion, thermogenesis, pain, growth, and other responses. The computational analysis identified a conserved amino acid sequence, supporting an evolutionary role of EREG as an alternative LepR ligand.
Schlagwörter epiregulin ; leptin receptor ; ERK ; EGFR ; glucose uptake ; energy metabolism ; Biology (General) ; QH301-705.5
Thema/Rubrik (Code) 570 ; 333
Sprache Englisch
Erscheinungsdatum 2022-01-01T00:00:00Z
Verlag MDPI AG
Dokumenttyp Artikel ; Online
Datenquelle BASE - Bielefeld Academic Search Engine (Lebenswissenschaftliche Auswahl)

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