首页> 美国卫生研究院文献>The Journal of Neuroscience >Prepubertal Development of GABAergic Transmission to Gonadotropin-Releasing Hormone (GnRH) Neurons and Postsynaptic Response Are Altered by Prenatal Androgenization
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Prepubertal Development of GABAergic Transmission to Gonadotropin-Releasing Hormone (GnRH) Neurons and Postsynaptic Response Are Altered by Prenatal Androgenization

机译:产前雄激素作用会改变GABA能传递到促性腺激素释放激素(GnRH)神经元的青春期前发育和突触后反应。

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摘要

Gonadotropin-releasing hormone (GnRH) neurons regulate reproduction through pulsatile GnRH release. Women with polycystic ovary syndrome (PCOS) have persistently elevated luteinizing hormone release frequency, reflecting GnRH release; this exacerbates hyperandrogenemia and disrupted reproductive cycles that are characteristic of this disorder. Clinical evidence suggests that neuroendocrine features of PCOS may manifest peripubertally. Adult mice prenatally exposed to androgens (PNA) mimic several reproductive features of PCOS. GnRH neurons from these mice have increased firing activity and receive increased GABAergic transmission, which is excitatory. When changes emerge during development is unknown. To study the typical postnatal development of GABAergic transmission and the effects of PNA treatment and sex, whole-cell voltage-clamp recordings were made of GABAergic postsynaptic currents (PSCs) in GnRH neurons in brain slices from prepubertal through adult control and PNA female and male mice. GABAergic transmission was present by 1 week of age in females and males and increased in frequency, reaching adult levels at 3 and 4 weeks, respectively. GABAergic PSC frequency was elevated in 3-week-old PNA versus control females. PSC frequency in both controls and PNA mice was activity independent, suggesting that PNA induces changes in synapse organization. PNA also alters the functional response of GnRH neurons to GABA. GABA induced firing in fewer neurons from 3-week-old PNA than control females; membrane potential depolarization induced by GABA was also reduced in cells from PNA mice at this age. PNA thus induces changes during development in the presynaptic organization of the GABAergic network afferent to GnRH neurons as well as the postsynaptic GnRH neuron response, both of which may contribute to adult reproductive dysfunction.>SIGNIFICANCE STATEMENT The central neuronal network that regulates reproduction is overactive in polycystic ovary syndrome (PCOS), a leading cause of infertility. Recent evidence of neuroendocrine dysfunction in midpubertal girls suggests that the pathophysiological mechanisms underlying PCOS may arise before pubertal maturation. Prenatal exposure to androgens (PNA) in mice mimics several neuroendocrine features of PCOS. GABAergic transmission to gonadotropin-releasing hormone (GnRH) neurons is important for reproduction and is increased in adult PNA mice. The typical development of this network and when changes with PNA and sex arise relative to puberty are unknown. These studies provide evidence that PNA alters prepubertal development of the GABAergic network afferent to GnRH neurons, including both the presynaptic organization and postsynaptic response. These changes may contribute to reproductive dysfunction in adults.
机译:促性腺激素释放激素(GnRH)神经元通过搏动性GnRH释放来调节生殖。多囊卵巢综合征(PCOS)妇女的黄体生成激素释放频率持续升高,反映了GnRH的释放。这加剧了高雄激素血症并破坏了这种疾病的特征性生殖周期。临床证据表明,PCOS的神经内分泌特征可能在青春期前表现出来。产前暴露于雄激素(PNA)的成年小鼠模仿了PCOS的几个生殖特征。这些小鼠的GnRH神经元具有增强的放电活性,并能增加GABA能传递,这是兴奋性的。在开发过程中何时出现变化是未知的。为了研究GABA能量传递的典型产后发展以及PNA治疗和性别的影响,对青春期前至成年对照以及PNA男女之间的大脑切片中GnRH神经元的GABA能突触后突触电流(PSC)进行了全细胞电压钳记录。老鼠。女性和男性在1周龄时就存在GABA能传递,并且频率增加,分别在3周和4周时达到成人水平。与对照组女性相比,在3周大的PNA中,GABA能的PSC频率升高。对照组和PNA小鼠的PSC频率均与活动无关,表明PNA诱导突触组织的变化。 PNA还改变了GnRH神经元对GABA的功能反应。 GABA诱导的3周龄PNA的神经元放电少于对照组女性。在这个年龄的PNA小鼠细胞中,GABA诱导的膜电位去极化也降低了。因此,PNA会在GnRH神经元传入的GABA能神经网络的突触前组织以及突触后GnRH神经元反应的发育过程中引起变化,这两者都可能导致成人生殖功能障碍。>意义声明多囊卵巢综合征(PCOS)是不孕症的主要原因,它调节生殖的作用过度。青春期中期女孩神经内分泌功能障碍的最新证据表明,PCOS的病理生理机制可能在青春期成熟之前出现。小鼠的产前暴露于雄激素(PNA)可以模仿PCOS的几种神经内分泌功能。 GABA能传递至促性腺激素释放激素(GnRH)神经元对于生殖至关重要,并且在成年PNA小鼠中会增加。该网络的典型发展以及与青春期有关的PNA和性别变化何时出现尚不清楚。这些研究提供了证据,表明PNA会改变GnRH神经元传入的GABA能网络的青春期前发育,包括突触前组织和突触后反应。这些变化可能导致成人生殖功能障碍。

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