| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 10873367 | FEBS Letters | 2005 | 6 Pages |
Abstract
Implantation of a fast growing tumour to mice (Lewis lung carcinoma) resulted in a clear cachectic state characterized by a profound muscle wasting. This was accompanied by a significant increase in both UCP2 and UCP3 gene expression in skeletal muscle and heart. Interestingly, this increase in gene expression was not linked to a rise in circulating fatty acids or in a decrease in food intake, as previously reported in other pathophysiological states. These results question the concept that hyperlipaemia is the only factor controlling UCP gene expression in different pathophysiological conditions. In addition, the present work suggests that UCPs might participate in a counter-regulatory mechanism to lower the production of ROS.
Keywords
LPSTNFUCPIL-15FFABATIL-1βEDLROSFree fatty acidFree fatty acidsextensor digitorum longusInterleukin-15Interleukin-1βWhite adipose tissuebrown adipose tissuetumour necrosis factor-αuncoupling protein-3Cancer cachexiaUncoupling Protein-2lipopolysaccharideNitric oxideUncoupling proteinWATReactive oxygen species
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Authors
SÃlvia Busquets, Vanessa Almendro, Esther Barreiro, Maite Figueras, Josep M. Argilés, Francisco J. López-Soriano,