PLoS ONE (Jan 2009)

Altered energy homeostasis and resistance to diet-induced obesity in KRAP-deficient mice.

  • Takahiro Fujimoto,
  • Kyoko Miyasaka,
  • Midori Koyanagi,
  • Toshiyuki Tsunoda,
  • Iwai Baba,
  • Keiko Doi,
  • Minoru Ohta,
  • Norihiro Kato,
  • Takehiko Sasazuki,
  • Senji Shirasawa

DOI
https://doi.org/10.1371/journal.pone.0004240
Journal volume & issue
Vol. 4, no. 1
p. e4240

Abstract

Read online

Obesity and related metabolic disorders have become leading causes of adult morbidity and mortality. KRAP (Ki-ras-induced actin-interacting protein) is a cytoskeleton-associated protein and a ubiquitous protein among tissues, originally identified as a cancer-related molecule, however, its physiological roles remain unknown. Here we demonstrate that KRAP-deficient (KRAP(-/-)) mice show enhanced metabolic rate, decreased adiposity, improved glucose tolerance, hypoinsulinemia and hypoleptinemia. KRAP(-/-) mice are also protected against high-fat diet-induced obesity and insulin resistance despite of hyperphagia. Notably, glucose uptake in the brown adipose tissue (BAT) in KRAP(-/-) mice is enhanced in an insulin-independent manner, suggesting that BAT is involved in altered energy homeostasis in KRAP(-/-) mice, although UCP (Uncoupling protein) expressions are not altered. Of interest is the down-regulation of fatty acid metabolism-related molecules, including acetyl-CoA carboxylase (ACC)-1, ACC-2 and fatty acid synthase in the liver of KRAP(-/-) mice, which could in part account for the metabolic phenotype in KRAP(-/-) mice. Thus, KRAP is a novel regulator in whole-body energy homeostasis and may be a therapeutic target in obesity and related diseases.