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Original Articles

Adaptations of Arginine's Intestinal-Renal Axis in Cachectic Tumor-Bearing Rats

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Pages 713-720 | Received 07 Mar 2014, Accepted 11 Feb 2015, Published online: 16 Apr 2015
 

Abstract

Malignancies induce disposal of arginine, an important substrate for the immune system. To sustain immune function, the tumor-bearing host accelerates arginine's intestinal-renal axis by glutamine mobilization from skeletal muscle and this may promote cachexia. Glutamine supplementation stimulates argi-nine production in healthy subjects. Arginine's intestinal-renal axis and the effect of glutamine supplementation in cancer cach-exia have not been investigated. This study evaluated the long-term adaptations of the interorgan pathway for arginine production following the onset of cachexia and the metabolic effect of glutamine supplementation in the cachectic state. Fischer-344 rats were randomly divided into a tumor-bearing group (n = 12), control group (n = 7) and tumor-bearing group receiving a glutamine-enriched diet (n = 9). Amino acid fluxes and net fractional extractions across intestine, kidneys, and liver were studied. Compared to controls, the portal-drained viscera of tumor-bearing rats took up significantly more glutamine and released significantly less citrulline. Renal metabolism was unchanged in the cachectic tumor-bearing rats compared with controls. Glutamine supplementation had no effects on intestinal and renal adaptations. In conclusion, in the cachectic state, an increase in intestinal glutamine uptake is not accompanied by an increase in renal arginine production. The adaptations found in the cachectic, tumor-bearing rat do not depend on glutamine availability.

FUNDING

This work was supported in part by a research grant to Nikki Buijs from the Vivax Foundation, “Food to Fight Cancer,” the Netherlands. The foundation did not participate in data collection, data analysis, data interpretation, writing, or submission of the article. Paul A. M. van Leeuwen reports receiving fees from Fresenius Medical Care for clinical consultation. Other authors disclose no potential conflict of interest.

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