Journal
ENDOCRINOLOGY
Volume 144, Issue 5, Pages 1753-1760Publisher
ENDOCRINE SOC
DOI: 10.1210/en.2002-221096
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Funding
- FIC NIH HHS [R03-TW-01233] Funding Source: Medline
- NIDA NIH HHS [F32-DA-05841] Funding Source: Medline
- NIDDK NIH HHS [P01-DK-55819, F32-DK-10082] Funding Source: Medline
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Proopiomelanocortin ( POMC) neurons in the hypothalamus are direct targets of the adipostatic hormone leptin and contribute to energy homeostasis by integrating peripheral and central information. The melanocortin and beta-endorphin neuropeptides are processed from POMC and putatively coreleased at axon terminals. Melanocortins have been shown by a combination of pharmacological and genetic methods to have inhibitory effects on appetite and body weight. In contrast, pharmacological studies have generally indicated that opioids stimulate food intake. Here we report that male mice engineered to selectively lack beta-endorphin, but that retained normal melanocortin signaling, were hyperphagic and obese. Furthermore, beta-endorphin mutant and wild-type mice had identical orexigenic responses to exogenous opioids and identical anorectic responses to the nonselective opioid antagonist naloxone, implicating an alternative endogenous opioid tone to beta-endorphin that physiologically stimulates feeding. These genetic data indicate that beta-endorphin is required for normal regulation of feeding, but, in contrast to earlier reports suggesting opposing actions of beta-endorphin and melanocortins on appetite, our results suggest a more complementary interaction between the endogenously released POMC-derived peptides in the regulation of energy homeostasis.
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