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下丘脑 - 垂体 - 性腺轴中食欲素A的相互作用。

Orexin A interactions in the hypothalamo-pituitary gonadal axis.

作者信息

Russell S H, Small C J, Kennedy A R, Stanley S A, Seth A, Murphy K G, Taheri S, Ghatei M A, Bloom S R

机构信息

Imperial College School of Medicine Endocrine Unit, Hammersmith Hospital, London W12 ONN, United Kingdom.

出版信息

Endocrinology. 2001 Dec;142(12):5294-302. doi: 10.1210/endo.142.12.8558.

DOI:10.1210/endo.142.12.8558
PMID:11713229
Abstract

The distribution of orexin A-immunoreactive neurons and orexin type I receptors in the CNS suggests important roles in regulating the hypothalamo-pituitary gonadal (HPG) axis and sexual behaviors. We examined orexin A interactions in the HPG axis in vivo and in vitro. Orexin A stimulated LH-releasing hormone (LHRH) release in hypothalamic explants harvested from male rats (+133%) and from females at proestrus (+233%), with no effect at estrus or metestrus. Orexin A dose dependently inhibited LHRH-stimulated LH release in dispersed pituitaries from proestrous females only. A selective NPY1-receptor antagonist abolished in vitro release of LHRH by orexin A. Hyperestrogenization in female rats reduced orexin A content in hypothalamus (-28%), midbrain (-26%), medulla (-40%), thalamus (-36%), olfactory tubercles (-25%), and cortex (-35%), brain regions that are important in HPG control and sex-cycle specific behaviors. Orexin A content was lower in hypothalamus (-20%) and higher in midbrain (+40%), medulla (+31%), and thalamus (+33%) at late proestrus vs. other cycle stages. Orexin A release after administration of 56 mM KCl was significantly greater in hypothalamic explants harvested on the morning of proestrus than at estrus or metestrus, and orexin A release was stimulated by estradiol (E2) in explants from males. These results reveal important interactions for orexin A in the HPG axis.

摘要

中枢神经系统中食欲素A免疫反应性神经元和食欲素I型受体的分布表明,它们在调节下丘脑-垂体-性腺(HPG)轴和性行为中发挥着重要作用。我们在体内和体外研究了食欲素A在HPG轴中的相互作用。食欲素A刺激了从雄性大鼠采集的下丘脑外植体中促黄体生成素释放激素(LHRH)的释放(增加133%),以及在动情前期雌性大鼠的下丘脑外植体中LHRH的释放(增加233%),而在发情期或发情后期则没有影响。食欲素A仅剂量依赖性地抑制动情前期雌性大鼠分散垂体中LHRH刺激的促黄体生成素释放。一种选择性神经肽Y1受体拮抗剂消除了食欲素A在体外对LHRH的释放作用。雌性大鼠的高雌激素化降低了下丘脑(-28%)、中脑(-26%)、延髓(-40%)、丘脑(-36%)、嗅结节(-25%)和皮质(-35%)中的食欲素A含量,这些脑区在HPG控制和性周期特异性行为中很重要。与其他周期阶段相比,在动情后期,下丘脑的食欲素A含量较低(-20%),而中脑(+40%)、延髓(+31%)和丘脑(+33%)中的食欲素A含量较高。在动情前期早晨采集的下丘脑外植体中,给予56 mM氯化钾后食欲素A的释放明显大于发情期或发情后期,并且在雄性大鼠的外植体中,雌二醇(E2)刺激了食欲素A的释放。这些结果揭示了食欲素A在HPG轴中的重要相互作用。

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