JCI Insight (Sep 2021)

Anterograde regulation of mitochondrial genes and FGF21 signaling by hepatic LSD1

  • Yang Cao,
  • Lingyi Tang,
  • Kang Du,
  • Kitt Paraiso,
  • Qiushi Sun,
  • Zhengxia Liu,
  • Xiaolong Ye,
  • Yuan Fang,
  • Fang Yuan,
  • Hank Chen,
  • Yumay Chen,
  • Xiaorong Wang,
  • Clinton Yu,
  • Ira L. Blitz,
  • Ping H. Wang,
  • Lan Huang,
  • Haibo Cheng,
  • Xiang Lu,
  • Ken W.Y. Cho,
  • Marcus Seldin,
  • Zhuyuan Fang,
  • Qin Yang

Journal volume & issue
Vol. 6, no. 17

Abstract

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Mitochondrial biogenesis and function are controlled by anterograde regulatory pathways involving more than 1000 nuclear-encoded proteins. Transcriptional networks controlling the nuclear-encoded mitochondrial genes remain to be fully elucidated. Here, we show that histone demethylase LSD1 KO from adult mouse liver (LSD1-LKO) reduces the expression of one-third of all nuclear-encoded mitochondrial genes and decreases mitochondrial biogenesis and function. LSD1-modulated histone methylation epigenetically regulates nuclear-encoded mitochondrial genes. Furthermore, LSD1 regulates gene expression and protein methylation of nicotinamide mononucleotide adenylyltransferase 1 (NMNAT1), which controls the final step of NAD+ synthesis and limits NAD+ availability in the nucleus. Lsd1 KO reduces NAD+-dependent SIRT1 and SIRT7 deacetylase activity, leading to hyperacetylation and hypofunctioning of GABPβ and PGC-1α, the major transcriptional factor/cofactor for nuclear-encoded mitochondrial genes. Despite the reduced mitochondrial function in the liver, LSD1-LKO mice are protected from diet-induced hepatic steatosis and glucose intolerance, partially due to induction of hepatokine FGF21. Thus, LSD1 orchestrates a core regulatory network involving epigenetic modifications and NAD+ synthesis to control mitochondrial function and hepatokine production.

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