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Publication : Eicosapentaenoic acid and oxypurinol in the treatment of muscle wasting in a mouse model of cancer cachexia.

First Author  Vaughan VC Year  2012
Journal  PLoS One Volume  7
Issue  9 Pages  e45900
PubMed ID  23029301 Mgi Jnum  J:191973
Mgi Id  MGI:5463707 Doi  10.1371/journal.pone.0045900
Citation  Vaughan VC, et al. (2012) Eicosapentaenoic acid and oxypurinol in the treatment of muscle wasting in a mouse model of cancer cachexia. PLoS One 7(9):e45900
abstractText  Cancer cachexia is a wasting condition, driven by systemic inflammation and oxidative stress. This study investigated eicosapentaenoic acid (EPA) in combination with oxypurinol as a treatment in a mouse model of cancer cachexia. Mice with cancer cachexia were randomized into 4 treatment groups (EPA (0.4 g/kg/day), oxypurinol (1 mmol/L ad-lib), combination, or control), and euthanized after 29 days. Analysis of oxidative damage to DNA, mRNA analysis of pro-oxidant, antioxidant and proteolytic pathway components, along with enzyme activity of pro- and antioxidants were completed on gastrocnemius muscle. The control group displayed earlier onset of tumor compared to EPA and oxypurinol groups (P<0.001). The EPA group maintained body weight for an extended duration (20 days) compared to the oxypurinol (5 days) and combination (8 days) groups (P<0.05). EPA (18.2+/-3.2 pg/ml) and combination (18.4+/-3.7 pg/ml) groups had significantly higher 8-OH-dG levels than the control group (12.9+/-1.4 pg/ml, P</=0.05) indicating increased oxidative damage to DNA. mRNA levels of GPx1, MURF1 and MAFbx were higher following EPA treatment compared to control (P</=0.05). Whereas oxypurinol was associated with higher GPx1, MnSOD, CAT, XDH, MURF1, MAFbx and UbB mRNA compared to control (P</=0.05). Activity of total SOD was higher in the oxypurinol group (32.2+/-1.5 U/ml) compared to control (27.0+/-1.3 U/ml, P<0.01), GPx activity was lower in the EPA group (8.76+/-2.0 U/ml) compared to control (14.0+/-1.9 U/ml, P<0.05), and catalase activity was lower in the combination group (14.4+/-2.8 U/ml) compared to control (20.9+/-2.0 U/ml, P<0.01). There was no change in XO activity. The increased rate of weight decline in mice treated with oxypurinol indicates that XO may play a protective role during the progression of cancer cachexia, and its inhibition is detrimental to outcomes. In combination with EPA, there was little significant improvement from control, indicating oxypurinol is unlikely to be a viable treatment compound in cancer cachexia.
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