Elevated energy expenditure in hepatocytes from tumor-bearing rats |
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Authors: | M S Roh L G Ekman M Jeevanandam M F Brennan |
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Affiliation: | Surgical Metabolism Laboratory, Memorial Sloan-Kettering Cancer Center, 1275 York Avenue, New York, New York 10021 USA |
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Abstract: | Mechanisms for the development of cancer cachexia are not well defined. Oxygen consumption and the capacity of the host liver to metabolize lactate were studied in isolated hepatocytes from sarcoma-bearing rats (TIH) and pair-fed controls (CH). Basal oxygen consumption (without exogenous substrate) is significantly increased by 65% in the TIH as compared to the CH. The addition of a physiologic concentration of lactate stimulated oxygen consumption over the already stimulated basal state by 13% in the TIH compared to 5% in the CH. When the hepatocytes are incubated with 1.5 mM of [U-14C]lactate, glucose production, lactate oxidation, and entry of lactate carbons into nonsecretory protein are significantly increased in the TIH. Associated with this stimulation is a significant decrease in lactate incorporation into glycogen and lipid in the TIH. This study suggests that the tumor-influenced liver utilizes lactate at an increased rate and its intermediary metabolism is directed toward energy utilization rather than energy storage. The enhanced metabolic processes in the tumor-influenced liver are associated with an increased oxygen consumption which may be a contributory factor to the negative energy balance, a characteristic of cancer cachexia. |
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Keywords: | To whom reprint requests should be addressed: Department of Surgery Memorial Sloan-Kettering Cancer Center 1275 York Avenue New York N. Y. 10021. |
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