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食欲素对生长激素分泌的体外调节作用。

The in vitro regulation of growth hormone secretion by orexins.

作者信息

Chen Chen, Xu Ruwei

机构信息

Prince Henry's Institute of Medical Research, and Department of Physiology, PO Box 5152, Monash University, Clayton, Victoria 3168, Australia.

出版信息

Endocrine. 2003 Oct;22(1):57-66. doi: 10.1385/ENDO:22:1:57.

DOI:10.1385/ENDO:22:1:57
PMID:14610299
Abstract

Orexins, orexigenic neuropeptides, have recently been discovered in lateral hypothalamus and play an important role in the regulation of pituitary hormone secretion. Two subtypes of orexin receptors (orexin-1 and orexin-2) have been demonstrated in pituitaries. In this experiment, the effects of orexins on voltage-gated Ca2+ currents and the GH release in primary cultured ovine somatotropes were examined. Voltage-gated Ca2+ currents were isolated in ovine somatotropes as L, T, and N currents using whole-cell patch-clamp techniques and specific Ca2+ channel blocker and toxin. Application of orexin-A or orexin-B (100 nM) significantly, dose-dependently, and reversibly increased only nifedipine-sensitive L-type Ca2+ current. Inhibitors of PKC (calphostin C, PKC inhibitory peptide) but not inhibitors of PKA (H89, PKA inhibitory peptide) cancelled the increase in the L current by orexins. Co-administration of orexin-A and GHRH (10 nM) showed an additive effect on the L current. Specific intracellular Ca2+-store-depleting reagent, thapsigargin (1 microM), did not affect the orexin-induced increase in the L current. Orexin-B alone slightly increased GH release and co-administration of orexin-A and GHRH synergistically stimulated GH secretion in vitro. It is therefore suggested that orexins may play an important role in regulating GHRH-stimulated GH secretion through an increase in the L-type Ca2+ current and the PKC-mediated signaling pathways in ovine somatotropes.

摘要

食欲素,即促食欲神经肽,最近在下丘脑外侧被发现,并且在垂体激素分泌的调节中发挥重要作用。垂体中已证实存在两种食欲素受体亚型(食欲素-1和食欲素-2)。在本实验中,研究了食欲素对原代培养的绵羊生长激素细胞中电压门控Ca2+电流及生长激素释放的影响。利用全细胞膜片钳技术以及特异性Ca2+通道阻滞剂和毒素,在绵羊生长激素细胞中分离出电压门控Ca2+电流,分为L、T和N电流。应用食欲素-A或食欲素-B(100 nM)可显著、剂量依赖性且可逆地增加仅对硝苯地平敏感的L型Ca2+电流。蛋白激酶C的抑制剂(钙泊三醇C、蛋白激酶C抑制肽)而非蛋白激酶A的抑制剂(H89、蛋白激酶A抑制肽)可消除食欲素引起的L电流增加。食欲素-A与生长激素释放激素(10 nM)共同给药对L电流显示出相加作用。特异性细胞内Ca2+储存耗竭剂毒胡萝卜素(1 microM)不影响食欲素诱导的L电流增加。单独使用食欲素-B可轻微增加生长激素释放,食欲素-A与生长激素释放激素共同给药在体外可协同刺激生长激素分泌。因此,提示食欲素可能通过增加绵羊生长激素细胞中的L型Ca2+电流以及蛋白激酶C介导的信号通路,在调节生长激素释放激素刺激的生长激素分泌中发挥重要作用。

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Orexin-B augments voltage-gated L-type Ca(2+) current via protein kinase C-mediated signalling pathway in ovine somatotropes.食欲素B通过蛋白激酶C介导的信号通路增强绵羊生长激素细胞中的电压门控L型Ca(2+)电流。
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Orexin-A augments voltage-gated Ca2+ currents and synergistically increases growth hormone (GH) secretion with GH-releasing hormone in primary cultured ovine somatotropes.食欲素A增强电压门控性Ca2+电流,并与生长激素释放激素协同增加原代培养的绵羊生长激素细胞中的生长激素(GH)分泌。
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Hypocretin-2 (orexin-B) modulation of superficial dorsal horn activity in rat.大鼠中下丘脑泌素-2(食欲素B)对脊髓背角浅层活动的调节
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