Scientific Reports (May 2017)

Mitochondrial retrograde signaling connects respiratory capacity to thermogenic gene expression

  • Minwoo Nam,
  • Thomas E. Akie,
  • Masato Sanosaka,
  • Siobhan M. Craige,
  • Shashi Kant,
  • John F. Keaney Jr,
  • Marcus P. Cooper

DOI
https://doi.org/10.1038/s41598-017-01879-x
Journal volume & issue
Vol. 7, no. 1
pp. 1 – 12

Abstract

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Abstract Mitochondrial respiration plays a crucial role in determining the metabolic state of brown adipose tissue (BAT), due to its direct roles in thermogenesis, as well as through additional mechanisms. Here, we show that respiration-dependent retrograde signaling from mitochondria to nucleus contributes to genetic and metabolic reprogramming of BAT. In mouse BAT, ablation of LRPPRC (LRP130), a potent regulator of mitochondrial transcription and respiratory capacity, triggers down-regulation of thermogenic genes, promoting a storage phenotype in BAT. This retrograde regulation functions by inhibiting the recruitment of PPARγ to the regulatory elements of thermogenic genes. Reducing cytosolic Ca2+ reverses the attenuation of thermogenic genes in brown adipocytes with impaired respiratory capacity, while induction of cytosolic Ca2+ is sufficient to attenuate thermogenic gene expression, indicating that cytosolic Ca2+ mediates mitochondria-nucleus crosstalk. Our findings suggest respiratory capacity governs thermogenic gene expression and BAT function via mitochondria-nucleus communication, which in turn leads to either a thermogenic or storage mode.