Frontiers in Endocrinology (May 2021)

Investigation of the Molecular Mechanisms by Which Endothelin-3 Stimulates Preadipocyte Growth

  • An-Ci Siao,
  • Li-Jane Shih,
  • Li-Jane Shih,
  • Yen-Yue Lin,
  • Yen-Yue Lin,
  • Yen-Yue Lin,
  • Yi-Wei Tsuei,
  • Yow-Chii Kuo,
  • Hui-Chen Ku,
  • Chih-Ping Chuu,
  • Po-Jen Hsiao,
  • Po-Jen Hsiao,
  • Po-Jen Hsiao,
  • Po-Jen Hsiao,
  • Yung-Hsi Kao

DOI
https://doi.org/10.3389/fendo.2021.661828
Journal volume & issue
Vol. 12

Abstract

Read online

Endothelins induce many biological responses, and they are composed of three peptides: ET-1, ET-2, and ET-3. Reports have indicated that ET-1 regulates cell proliferation, adipogenesis, and other cell responses and that ET-3 stimulates the growth of gastrointestinal epithelial cells and melanocytes. However, the signalling pathways of ET3 that mediate the growth of fat cells are still unclear. Using 3T3-L1 white preadipocytes, we found that ET-3 induced increases in both cell number and BrdU incorporation. Pretreatment with an ETAR antagonist (but not an ETBR antagonist) blocked the ET-3-induced increases in both cell number and BrdU incorporation. Additionally, BQ610 suppressed the ET-3-induced increases in phosphorylation of AMPK, c-JUN, and STAT3 proteins, and pretreatment with specific inhibitors of AMPK, JNK/c-JUN, or JAK/STAT3 prevented the ET-3-induced increases in phosphorylation of AMPK, c-JUN, and STAT3, respectively. Neither p38 MAPK inhibitor nor PKC inhibitor altered the effects of ET-3 on cell growth. These data suggest that ET-3 stimulates preadipocyte growth through the ETAR, AMPK, JNK/c-JUN, and STAT3 pathways. Moreover, ET-3 did not alter HIB1B brown preadipocyte and D12 beige preadipocyte growth, suggesting a preadipocyte type-dependent effect. The results of this study may help explain how endothelin mediates fat cell activity and fat cell-associated diseases.

Keywords