4.5 Article

Prolonged food deprivation increases mRNA expression of deiodinase 1 and 2, and thyroid hormone receptor β-1 in a fasting-adapted mammal

Journal

JOURNAL OF EXPERIMENTAL BIOLOGY
Volume 216, Issue 24, Pages 4647-4654

Publisher

COMPANY OF BIOLOGISTS LTD
DOI: 10.1242/jeb.085290

Keywords

lipid metabolism; reverse T3; seal; thyroxine; triiodothyronine

Categories

Funding

  1. University of California Institute for Mexico
  2. United States and Mexico's National Council for Science and Technology (UC MEXUS CONACYT)
  3. UC MEXUS, CONACYT
  4. University of California (Miguel Velez Fellowship, UC Merced GRC)
  5. National Institutes of Health (NIH) National Heart, Lung and Blood Institute (NHLBI) [NIH NHLBI R01HL09176-S]
  6. NHLBI [K02HL103787]
  7. NIH NHLBI [R01HL09176]

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Food deprivation in mammals is typically associated with reduced thyroid hormone (TH) concentrations and deiodinase content and activity to suppress metabolism. However, in prolonged-fasted, metabolically active elephant seal pups, TH levels are maintained, if not elevated. The functional relevance of this apparent paradox is unknown and demonstrates variability in the regulation of TH levels, metabolism and function in food-deprived mammals. To address our hypothesis that cellular TH-mediated activity is upregulated with fasting duration, we quantified the mRNA expression and protein content of adipose and muscle deiodinase type I (DI1) and type II (DI2), and TH receptor beta-1 (THr beta-1) after 1, 3 and 7 weeks of fasting in northern elephant seal pups (N= 5-7 per week). Fasting did not decrease the concentrations of plasma thyroid stimulating hormone, total triiodothyronine (tT(3)), free T-3, total thyroxine (tT(4)) or free T-4, suggesting that the hypothalamic-pituitary-thyroid axis is not suppressed, but rather maintained during fasting. Mean mRNA expression of adipose DI1 and DI2 increased threefold and fourfold, respectively, and 20 and 30-fold, respectively, in muscle. With the exception of adipose DI1, protein expression of adipose DI2 and muscle DI1 and DI2 increased twofold to fourfold. Fasting also increased adipose (fivefold) and muscle (fourfold) THr beta-1 mRNA expression, suggesting that the mechanisms mediating cellular TH activity are upregulated with prolonged fasting. The data demonstrate a unique, atypical mechanism of TH activity and regulation in mammals adapted to prolonged food deprivation in which the potential responsiveness of peripheral tissues and cellular TH activity are increased, which may contribute to their lipid-based metabolism.

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