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FSP27 contributes to efficient energy storage in murine white adipocytes by promoting the formation of unilocular lipid droplets

Authors :
Yasushi Matsuki
Sohei Kitazawa
Masayuki Saito
Hitoshi Okamura
Takayuki Kawaguchi
Atsu Aiba
Yoshikazu Tamori
Takashi Osumi
Satoru Masubuchi
Kazuki Nakao
Toyoshi Fujimoto
Riko Kitazawa
Taku Amo
Sanshiro Tateya
Wataru Mizunoya
Shigeo Ohta
Jinglei Cheng
Tohru Fushiki
Tomohiro Yamaguchi
Asako Omachi
Tetsuro Shibakusa
Kazuhiro Kimura
Masato Kasuga
Naonobu Nishino
Kazuo Inoue
Harumi Nakao
Ryuji Hiramatsu
Source :
Journal of Clinical Investigation.
Publication Year :
2008
Publisher :
American Society for Clinical Investigation, 2008.

Abstract

White adipocytes are unique in that they contain large unilocular lipid droplets that occupy most of the cytoplasm. To identify genes involved in the maintenance of mature adipocytes, we expressed dominant-negative PPARĪ³ in 3T3-L1 cells and performed a microarray screen. The fat-specific protein of 27 kDa (FSP27) was strongly downregulated in this context. FSP27 expression correlated with induction of differentiation in cultured preadipocytes, and the protein localized to lipid droplets in murine white adipocytes in vivo. Ablation of FSP27 in mice resulted in the formation of multilocular lipid droplets in these cells. Furthermore, FSP27-deficient mice were protected from diet-induced obesity and insulin resistance and displayed an increased metabolic rate due to increased mitochondrial biogenesis in white adipose tissue (WAT). Depletion of FSP27 by siRNA in murine cultured white adipocytes resulted in the formation of numerous small lipid droplets, increased lipolysis, and decreased triacylglycerol storage, while expression of FSP27 in COS cells promoted the formation of large lipid droplets. Our results suggest that FSP27 contributes to efficient energy storage in WAT by promoting the formation of unilocular lipid droplets, thereby restricting lipolysis. In addition, we found that the nature of lipid accumulation in WAT appears to be associated with maintenance of energy balance and insulin sensitivity.

Details

ISSN :
00219738
Database :
OpenAIRE
Journal :
Journal of Clinical Investigation
Accession number :
edsair.doi...........dd0f29f72a6daf3967267cbf438d9649
Full Text :
https://doi.org/10.1172/jci34090