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促性腺激素释放激素(GnRH)神经元对通过I型GnRH受体介导的GnRH的反应呈剂量依赖性转变。

Dose-dependent switch in response of gonadotropin-releasing hormone (GnRH) neurons to GnRH mediated through the type I GnRH receptor.

作者信息

Xu Chun, Xu Xu-Zhi, Nunemaker Craig S, Moenter Suzanne M

机构信息

Department of Internal Medicine, P.O. Box 800578, University of Virginia, Charlottesville, VA 22908, USA.

出版信息

Endocrinology. 2004 Feb;145(2):728-35. doi: 10.1210/en.2003-0562. Epub 2003 Oct 23.

Abstract

Pulsatile release of GnRH provides central control of reproduction. GnRH neuron activity is likely synchronized to produce hormone pulses, but the mechanisms are largely unknown. One candidate for communication among these neurons is GnRH itself. Cultured embryonic and immortalized GnRH neurons express GnRH receptor type I (GnRHR-1), but expression has not been shown in adult GnRH neurons. Using mice that express green fluorescent protein (GFP) in GnRH neurons, we tested whether adult GnRH neurons express GnRHR-1. GFP-positive (n = 42) and -negative neurons (n = 22) were harvested from brain slices, and single-cell RT-PCR was performed with cell contents. Fifty-two percent of the GnRH neurons tested expressed GnRHR-1, but only 9% of non-GnRH hypothalamic neurons expressed GnRHR-1; no false harvest controls (n = 13) were positive. GnRHR-1 expression within GnRH neurons suggested a physiological ultrashort loop feedback role for GnRH. Thus, we examined the effect of GnRH on the firing rate of GnRH neurons. Low-dose GnRH (20 nm) significantly decreased firing rate in 12 of 22 neurons (by 42 +/- 4%, P < 0.05), whereas higher doses increased firing rate (200 nm, five of 10 neurons, 72 +/- 26%; 2000 nm, nine of 13 neurons, 53 +/- 8%). Interestingly, the fraction of GnRH neurons responding was similar to the fraction in which GnRHR-1 was detected. Together, these data demonstrate that a subpopulation of GnRH neurons express GnRHR-1 and respond to GnRH with altered firing. The dose dependence suggests that this autocrine control of GnRH neurons may be not only a mechanism for generating and modulating pulsatile release, but it may also be involved in the switch between pulse and surge modes of release.

摘要

促性腺激素释放激素(GnRH)的脉冲式释放对生殖起着中枢控制作用。GnRH神经元活动可能同步以产生激素脉冲,但其机制大多未知。这些神经元之间进行通讯的一个候选物质是GnRH本身。培养的胚胎和永生化GnRH神经元表达I型GnRH受体(GnRHR-1),但在成年GnRH神经元中尚未显示有该表达。利用在GnRH神经元中表达绿色荧光蛋白(GFP)的小鼠,我们测试了成年GnRH神经元是否表达GnRHR-1。从脑片中收集GFP阳性(n = 42)和阴性神经元(n = 22),并对细胞内容物进行单细胞逆转录聚合酶链反应(RT-PCR)。所测试的GnRH神经元中有52%表达GnRHR-1,但非GnRH下丘脑神经元中只有9%表达GnRHR-1;无假收获对照(n = 13)为阳性。GnRH神经元内的GnRHR-1表达提示GnRH具有生理超短环反馈作用。因此,我们研究了GnRH对GnRH神经元放电频率的影响。低剂量GnRH(20 nM)使22个神经元中的12个放电频率显著降低(降低42±4%,P < 0.05),而较高剂量则增加放电频率(200 nM,10个神经元中的5个,增加72±26%;2000 nM,13个神经元中的9个,增加53±8%)。有趣的是,对GnRH有反应的GnRH神经元比例与检测到GnRHR-1的比例相似。总之,这些数据表明一部分GnRH神经元表达GnRHR-1并对GnRH产生反应,其放电发生改变。剂量依赖性表明这种GnRH神经元的自分泌控制可能不仅是产生和调节脉冲式释放的一种机制,还可能参与释放的脉冲模式和激增模式之间的转换。

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