Different physiological roles of insulin receptors in mediating nutrient metabolism in zebrafish

Bin Yuan Yang, Gang Zhai, Yu Long Gong, Jing Zhi Su, Xu Yan Peng, Guo Hui Shang, Dong Han, Jun Yan Jin, Hao Kun Liu, Zhen Yu Du, Zhan Yin, Shou Qi Xie

Research output: Contribution to journalArticlepeer-review

49 Scopus citations

Abstract

Insulin, the most potent anabolic hormone, is critical for somatic growth and metabolism in vertebrates. Type 2 diabetes, which is the primary cause of hyperglycemia, results from an inability of insulin to signal glycolysis and gluconeogenesis. Our previous study showed that double knockout of insulin receptor a (insra) and b (insrb) caused β-cell hyperplasia and lethality from 5 to 16 days postfertilization (dpf) (Yang BY, Zhai G, Gong YL, Su JZ, Han D, Yin Z, Xie SQ. Sci Bull (Beijing) 62: 486–492, 2017). In this study, we characterized the physiological roles of Insra and Insrb, in somatic growth and fueling metabolism, respectively. A high-carbohydrate diet was provided for insulin receptor knockout zebrafish from 60 to 120 dpf to investigate phenotype inducement and amplification. We observed hyperglycemia in both insra–/– fish and insrb–/– fish. Impaired growth hormone signaling, increased visceral adiposity, and fatty liver were detected in insrb–/– fish, which are phenotypes similar to the lipodystrophy observed in mammals. More importantly, significantly diminished protein levels of P-PPARα, P-STAT5, and IGF-1 were also observed in insrb–/– fish. In insra–/– fish, we observed increased protein content and decreased lipid content of the whole body. Taken together, although Insra and Insrb show overlapping roles in mediating glucose metabolism through the insulin-signaling pathway, Insrb is more prone to promoting lipid catabolism and protein synthesis through activation of the growth hormone-signaling pathway, whereas Insra primarily acts to promote lipid synthesis via glucose utilization.

Original languageEnglish
Pages (from-to)E38-E51
JournalAmerican Journal of Physiology - Endocrinology and Metabolism
Volume315
Issue number1
DOIs
StatePublished - Jul 2018

Keywords

  • GH signaling
  • Hyperglycemia
  • Insulin receptors
  • Lipid metabolism

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