Abstract
We have developed a murine model of wasting by injecting intracerebrally cells which continuously secrete h-cachectin/ TNF (CHO-TNF) to: (a) determine the effects of cachectin/ TNF produced continuously in the central nervous system (CNS), and (b) compare the metabolic effects of cachectin/ TNF-secreting tumor in the brain to the cachexia caused by CHO-TNF tumor in peripheral tissue (IM). Intracerebral CHO-TNF tumors produced increased serum h-cachectin/ TNF levels with lethal hypophagia and weight loss (mean survival time of 11 d); these changes were not observed in association with nonsecretory control brain tumors. The metabolic consequences of intracerebral cachectin/TNF production were indistinguishable from acute, lethal starvation: whole-body lipid content was decreased significantly but protein was conserved. Although intramuscular cachectin/TNF-secreting tumors caused similar increases of serum h-cachectin/TNF levels, profound anorexia did not develop; wasting developed after a longer period of tumor burden (50 d) with classical signs of cachexia (i.e., anemia and depletion of both protein and lipid). These studies provide a reproducible animal model of site-specific cytokine production and suggest that, regardless of serum levels, cachectin/TNF produced locally in brain influences both the rate of development of wasting and its net metabolic effects.
Original language | English |
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Pages (from-to) | 2014-2024 |
Number of pages | 11 |
Journal | Journal of Clinical Investigation |
Volume | 86 |
Issue number | 6 |
State | Published - Dec 1990 |
Externally published | Yes |
Keywords
- AIDS
- Angiogenesis
- Anorexia
- Body composition
- Brain tumor
- Cancer
- Cytokines
- Tumor necrosis factor