[HTML][HTML] Abrogation of growth hormone secretion rescues fatty liver in mice with hepatocyte-specific deletion of JAK2

BC Sos, C Harris, SM Nordstrom… - The Journal of …, 2011 - Am Soc Clin Investig
BC Sos, C Harris, SM Nordstrom, JL Tran, M Balázs, P Caplazi, M Febbraio, MAB Applegate…
The Journal of clinical investigation, 2011Am Soc Clin Investig
Non-alcoholic fatty liver disease is associated with multiple comorbid conditions, including
diabetes, obesity, infection, and malnutrition. Mice with hepatocyte-specific disruption of
growth hormone (GH) signaling develop fatty liver (FL), although the precise mechanism
underlying this finding remains unknown. Because GH signals through JAK2, we developed
mice bearing hepatocyte-specific deletion of JAK2 (referred to herein as JAK2L mice). These
mice were lean, but displayed markedly elevated levels of GH, liver triglycerides (TGs), and …
Non-alcoholic fatty liver disease is associated with multiple comorbid conditions, including diabetes, obesity, infection, and malnutrition. Mice with hepatocyte-specific disruption of growth hormone (GH) signaling develop fatty liver (FL), although the precise mechanism underlying this finding remains unknown. Because GH signals through JAK2, we developed mice bearing hepatocyte-specific deletion of JAK2 (referred to herein as JAK2L mice). These mice were lean, but displayed markedly elevated levels of GH, liver triglycerides (TGs), and plasma FFAs. Because GH is known to promote lipolysis, we crossed GH-deficient little mice to JAK2L mice, and this rescued the FL phenotype. Expression of the fatty acid transporter CD36 was dramatically increased in livers of JAK2L mice, as was expression of Pparg. Since GH signaling represses PPARγ expression and Cd36 is a known transcriptional target of PPARγ, we treated JAK2L mice with the PPARγ-specific antagonist GW9662. This resulted in reduced expression of liver Cd36 and decreased liver TG content. These results provide a mechanism for the FL observed in mice with liver-specific disruption in GH signaling and suggest that the development of FL depends on both GH-dependent increases in plasma FFA and increased hepatic uptake of FFA, likely mediated by increased expression of CD36.
The Journal of Clinical Investigation