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Submitted on April 19, 2005
Accepted on August 18, 2005
Department of Cell Biology, Physiology and Immunology (M.L.B., R.P., F.G., J.M.C., L.P., E.A., M.T.-S.), University of Córdoba, 14004 Córdoba, Spain; Department of Histology and Pathology (M.A.B., M.A.), University of Navarra, 31080 Pamplona, Spain; Department of Physiology (C.D.), University of Santiago de Compostela, 15705 Santiago de Compostela, Spain; and Departments of Physiology and Pediatrics (H.H., M.N., J.T.), University of Turku, 20520 Turku, Finland
* To whom correspondence should be addressed. E-mail: fi1tesem{at}uco.es.
Orexins, hypothalamic neuropeptides initially involved in the control of food intake and sleep-wake cycle, have recently emerged as pleiotropic regulators of different biological systems, including the reproductive axis. Besides central actions, peripheral expression and functions of orexins have been reported, and prepro-orexin and orexin type-1 receptor mRNAs have been detected in the testis. However, the pattern of expression and biological actions of orexin in the male gonad remain mostly unexplored. We report herein analyses on testicular prepro-orexin mRNA expression and orexin-A immunoreactivity in different experimental settings, and on direct effects of orexin-A on seminiferous tubule functions. Expression of prepro-orexin mRNA was demonstrated in the rat testis at different stages of postnatal development, with negligible levels at early juvenile period and maximum values in adulthood. Likewise, orexin-A immunoreactivity was demonstrated along postnatal maturation, with strong peptide signal in Leydig cells and spermatocytes at specific stages of meiosis. Testicular expression of prepro-orexin mRNA appeared hormonally regulated: its levels decreased after hypophysectomy and increased following gonadotropin replacement and ghrelin stimulation. Finally, orexin-A suppressed the expression of key Sertoli cell genes, such as Müllerian-inhibiting substance and stem cell factor, and inhibited DNA synthesis in specific stages of the seminiferous epithelium. In conclusion, we provide evidence for the regulated expression of orexin in the rat testis, and its potential involvement in the control of seminiferous tubule functions. Together with our recent results on the expression of orexin type-1 receptor in the rat testis, our data further document a novel testicular site of action of orexins in the control of male reproductive axis.
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