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Mitochondrial pyruvate carrier is required for optimal brown fat thermogenesis.

Authors :
Panic V
Pearson S
Banks J
Tippetts TS
Velasco-Silva JN
Lee S
Simcox J
Geoghegan G
Bensard CL
van Ry T
Holland WL
Summers SA
Cox J
Ducker GS
Rutter J
Villanueva CJ
Source :
ELife [Elife] 2020 Aug 14; Vol. 9. Date of Electronic Publication: 2020 Aug 14.
Publication Year :
2020

Abstract

Brown adipose tissue (BAT) is composed of thermogenic cells that convert chemical energy into heat to maintain a constant body temperature and counteract metabolic disease. The metabolic adaptations required for thermogenesis are not fully understood. Here, we explore how steady state levels of metabolic intermediates are altered in brown adipose tissue in response to cold exposure. Transcriptome and metabolome analysis revealed changes in pathways involved in amino acid, glucose, and TCA cycle metabolism. Using isotopic labeling experiments, we found that activated brown adipocytes increased labeling of pyruvate and TCA cycle intermediates from U <superscript>13</superscript> C-glucose. Although glucose oxidation has been implicated as being essential for thermogenesis, its requirement for efficient thermogenesis has not been directly tested. We show that mitochondrial pyruvate uptake is essential for optimal thermogenesis, as conditional deletion of Mpc1 in brown adipocytes leads to impaired cold adaptation. Isotopic labeling experiments using U <superscript>13</superscript> C-glucose showed that loss of MPC1 led to impaired labeling of TCA cycle intermediates. Loss of MPC1 in BAT increased 3-hydroxybutyrate levels in blood and BAT in response to the cold, suggesting that ketogenesis provides an alternative fuel source to compensate. Collectively, these studies highlight that complete glucose oxidation is essential for optimal brown fat thermogenesis.<br />Competing Interests: VP, SP, JB, TT, JV, SL, JS, GG, CB, Tv, WH, SS, JC, GD, JR, CV No competing interests declared<br /> (© 2020, Panic et al.)

Details

Language :
English
ISSN :
2050-084X
Volume :
9
Database :
MEDLINE
Journal :
ELife
Publication Type :
Academic Journal
Accession number :
32795388
Full Text :
https://doi.org/10.7554/eLife.52558