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Growth Hormone Increases mRNA Levels of PPAR delta and Foxo1 in Skeletal Muscle of Growth Hormone Deficient lit/lit Mice

Authors
Kim, Dong-SunItoh, EminaIida, KeijiThorner, Michael O.
Issue Date
Feb-2009
Publisher
JAPAN ENDOCRINE SOC
Keywords
Growth hormone; Foxo1; PPAR-delta; Skeletal muscle
Citation
ENDOCRINE JOURNAL, v.56, no.1, pp.141 - 147
Indexed
SCIE
SCOPUS
Journal Title
ENDOCRINE JOURNAL
Volume
56
Number
1
Start Page
141
End Page
147
URI
https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/177317
DOI
10.1507/endocrj.K08E-219
ISSN
0918-8959
Abstract
GH plays an important role in lipid metabolism as a partitioning hormone. PPAR delta regulates lipid oxidation in skeletal muscle and is activated by several physiological ligands including fatty acids. To investigate whether GH has an effect on the regulation of transcription of PPAR delta and other genes involved in energy metabolism in skeletal muscle, mRNA levels were studied by real-time RT-PCR in lit/lit mice (isolated GH deficiency) and lit/+ mice controls (normal GH levels). Mice received either a single bolus (120 ng/g) of rat GH or vehicle, and skeletal muscle was collected 4h later. PPAR delta mRNA was increased in vehicle-treated lit/lit mice compared to vehicle-treated lit/+ mice (1.67 fold, P<0.05). lit/lit mice treated with GH showed a further increase in PPAR delta mRNA levels (2.83 fold vs. vehicle-treated lit/+ mice, P<0.001). mRNA levels of Foxo1 were increased in vehicle-treated lit/lit mice compared to vehicle-treated lit/+ mice (1.74 fold, P<0.05). lit/lit mice treated with GH showed a further increase in Foxo1 mRNA levels (6.30 fold vs. vehicle-treated lit/+ mice, P<0.001). mRNA levels of acyl CoA-oxidase showed a trend to be higher in vehicle-treated lit/lit mice compared to vehicle-treated lit/+ mice. This reached statistical significance in GH-treated lit/lit mice compared to vehicle-treated lit/+ mice (2.11 fold, P<0.05). In summary, mRNA levels of PPAR delta and Foxo1 were increased in skeletal muscle of GH-deficient mice, and further acutely increased by GH administration. These results suggest that GH plays a relevant role in the lipid catabolism in skeletal muscle.
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