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Netrin-1 通过依赖钙的方式刺激发育中的 GnRH 神经元向正中隆起延伸轴突。

Netrin-1 stimulates developing GnRH neurons to extend neurites to the median eminence in a calcium- dependent manner.

机构信息

Centre for Neuroendocrinology, Department of Anatomy, University of Otago, School of Medical Sciences, Dunedin, New Zealand.

出版信息

PLoS One. 2012;7(10):e46999. doi: 10.1371/journal.pone.0046999. Epub 2012 Oct 9.

Abstract

Hypothalamic gonadotropin-releasing hormone (GnRH) neurons are required for fertility in all mammalian species studied to date. In rodents, GnRH neuron cell bodies reside in the rostral hypothalamus, and most extend a single long neuronal process in the caudal direction to terminate at the median eminence (ME), the site of hormone secretion. The molecular cues that GnRH neurites use to grow and navigate to the ME during development, however, remain poorly described. Reverse transcription-PCR (RT-PCR) identified mRNAs encoding Netrin-1, and its receptor, DCC, in the fetal preoptic area (POA) and mediobasal hypothalamus (MBH), respectively, from gestational day 12.5 (GD12.5), a time when the first GnRH neurites extend toward the MBH. Moreover, a subpopulation of GnRH neurons from GD14.5 through GD18.5 express the Netrin-1 receptor, DCC, suggesting a role for Netrin-1/DCC signaling in GnRH neurite growth and/or guidance. In support of this notion, when GD15.5 POA explants, containing GnRH neurons actively extending neurites, were grown in three-dimensional collagen gels and challenged with exogenous Netrin-1 (100 ng/ml or 400 ng/ml) GnRH neurite growth was stimulated. In addition, Netrin-1 provided from a fixed source was able to stimulate outgrowth, although it did not appear to chemoattract GnRH neurites. Finally, the effects of Netrin-1 on the outgrowth of GnRH neurites could be inhibited by blocking either L-type voltage-gated calcium channels (VGCCs) with nifedipine (10 µM), or ryanodine receptors with ryanodine (10 µM). This is consistent with the role of Ca2+ from extra- and intracellular sources in Netrin-1/DCC-dependent growth cone motility in other neurons. These results indicate that Netrin-1 directly stimulates the growth of a subpopulation of GnRH neurites that express DCC, provide further understanding of the mechanisms by which GnRH nerve terminals arrive at their site of hormone secretion, and identify an additional neuronal population whose neurites utilize Netrin-1/DCC signaling for their development.

摘要

下丘脑促性腺激素释放激素 (GnRH) 神经元是迄今为止研究的所有哺乳动物物种生育所必需的。在啮齿动物中,GnRH 神经元胞体位于下丘脑的前部,大多数向尾部方向延伸单个长的神经元过程,终止于正中隆起(ME),这是激素分泌的部位。然而,GnRH 神经突在发育过程中用于生长和导航到 ME 的分子线索仍描述不足。逆转录 -PCR (RT-PCR) 从妊娠第 12.5 天 (GD12.5) 鉴定了编码 Netrin-1 的 mRNA,并分别在胎儿前脑区 (POA) 和中基底下丘脑 (MBH) 中鉴定了编码 Netrin-1 的受体 DCC,此时第一批 GnRH 神经突向 MBH 延伸。此外,从 GD14.5 到 GD18.5 的 GnRH 神经元的一个亚群表达 Netrin-1 受体 DCC,这表明 Netrin-1/DCC 信号在 GnRH 神经突生长和/或导向中起作用。支持这一观点,当包含 GnRH 神经元的 GD15.5 POA 外植体积极延伸神经突的 GD15.5 POA 外植体在三维胶原凝胶中生长并受到外源性 Netrin-1(100ng/ml 或 400ng/ml)的挑战时, GnRH 神经突的生长受到刺激。此外,来自固定源的 Netrin-1 能够刺激生长,但它似乎没有趋化 GnRH 神经突。最后,Netrin-1 对 GnRH 神经突生长的影响可以通过用硝苯地平 (10μM) 阻断 L 型电压门控钙通道 (VGCC) 或用钌红 (10μM) 阻断肌醇 1,4,5-三磷酸受体来抑制。这与其他神经元中 Netrin-1/DCC 依赖性生长锥运动中外源和细胞内 Ca2+ 的作用一致。这些结果表明,Netrin-1 直接刺激表达 DCC 的 GnRH 神经突的一个亚群的生长,进一步了解 GnRH 神经末梢到达其激素分泌部位的机制,并确定另一个神经元群体,其神经突利用 Netrin-1/DCC 信号进行发育。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7b70/3467286/65296c3eee5c/pone.0046999.g001.jpg

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