์ฝ˜ํ…์ธ ๋กœ ๊ฑด๋„ˆ๋›ฐ๊ธฐ
Merck

Metabolic nuclear receptors coordinate energy metabolism to regulate Sox9+ hepatocyte fate.

iScience (2021-09-11)
Shenghui Liu, Dan Qin, Yi Yan, Jiayan Wu, Lihua Meng, Wendong Huang, Liqiang Wang, Xiangmei Chen, Lisheng Zhang
์ดˆ๋ก

Recent research has indicated the adult liver Sox9+ cells located in the portal triads contribute to the physiological maintenance of liver mass and injury repair. However, the physiology and pathology regulation mechanisms of adult liver Sox9+ cells remain unknown. Here, PPARฮฑ and FXR bound to the shared site inย Sox9 promoter with opposite transcriptional outputs. PPARฮฑ activation enhanced the fatty acid ฮฒ-oxidation, oxidative phosphorylation (OXPHOS), and adenosine triphosphate (ATP) production, thus promoting proliferation and differentiation of Sox9+ hepatocytes along periportal (PP)-perivenous (PV) axis. However, FXR activation increased glycolysis but decreased OXPHOS and ATPย production, therefore preventing proliferation of Sox9+ hepatocytes along PP-PV axis by promoting Sox9+ hepatocyte self-renewal. Our research indicates that metabolic nuclear receptors play critical roles in liver progenitor Sox9+ hepatocyte homeostasis to initiate or terminate liver injury-induced cell proliferation and differentiation, suggesting that PPARฮฑ and FXR are potential therapeutic targets for modulating liver regeneration.

MATERIALS
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