Testosterone regulates pro-opiomelanocortin gene expression in the primate brain
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Authors
Steiner, Robert A.
Clifton, Donald K.
Adams, Lizabeth A.
Vician, Linda
Journal Title
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Publisher
Endocrine Society
Abstract
Endogenous opioid peptides such as beta-endorphin, derived from
proopiomelanocortin (POMC), have been widely implicated as serving an
important role in the neuroendocrine regulation of the primate
reproductive axis. In both human and nonhuman primates, POMC neurons are
thought to mediate, at least in part, the negative feedback action of sex
steroids on GnRH. Sex steroids, such as testosterone, are thought to
inhibit GnRH secretion by enhancing the inhibitory activity of
beta-endorphin; however, the cellular mechanisms by which steroid hormones
regulate the activity of POMC neurons in the primate brain are unknown. In
this study, we tested the hypothesis that testosterone stimulates POMC
gene expression within the primate brain and that this regulation occurs
within a specific subset of POMC neurons residing in the arcuate nucleus
of the hypothalamus. We used in situ hybridization to compare cellular
levels of POMC messenger RNA in intact (n = 4), castrated (n = 4), and
castrated/testosterone-treated (n = 4) monkeys. We report that after
castration of the male macaque (Macaca fascicularis), cellular POMC
messenger RNA levels decline significantly (P less than 0.05) in neurons
within the arcuate nucleus and that this decline is prevented by
replacement with physiological doses of testosterone. Moreover, we found
that this testosterone-dependent modulation of POMC gene expression is
restricted to a small fraction of the numerous POMC neurons located within
the most anterior region of the arcuate nucleus in the brain of this
primate species. These observations provide evidence that sex steroids
regulate expression of the POMC gene in the primate brain.
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Citation
Endocrinology. 1991 Apr;128(4):1881-6
