It has been earlier proposed that oxytocin could play a facilitatory role in the preovulatory LH surge in both rats and humans. We here provide evidence that oxytocin also facilitates sexual maturation in female rats. The administration of an oxytocin antagonist for 6 d to immature female rats decreased GnRH pulse frequency ex vivo and delayed the age at vaginal opening and first estrus. The in vitro reduction in GnRH pulse frequency required chronic blockade of oxytocin receptors, because it was not acutely observed after a single injection of the antagonist. Hypothalamic explants exposed to the antagonist in vitro showed a reduced GnRH pulse frequency and failed to respond to oxytocin with GnRH release. Prostaglandin E(2) (PGE(2)) mimicked the stimulatory effect of oxytocin on GnRH pulse frequency, and inhibition of PG synthesis blocked the effect of oxytocin, suggesting that oxytocin accelerates pulsatile GnRH release via PGE(2). The source of PGE(2) appears to be astrocytes, because oxytocin stimulates PGE(2) release from cultured hypothalamic astrocytes. Moreover, astrocytes express oxytocin receptors, whereas GnRH neurons do not. These results suggest that oxytocin facilitates female sexual development and that this effect is mediated by a mechanism involving glial production of PGE(2).

译文

早先有人提出,催产素可以在大鼠和人类的排卵前LH激增中起促进作用。我们在这里提供的证据表明催产素也促进雌性大鼠的性成熟。对未成熟的雌性大鼠施用催产素拮抗剂6 d可降低体外GnRH脉冲频率,并延迟阴道开放和首次发情的年龄。GnRH脉冲频率的体外降低需要长期阻断催产素受体,因为在单次注射拮抗剂后未观察到。体外暴露于拮抗剂的下丘脑外植体显示出GnRH脉冲频率降低,并且对GnRH释放的催产素没有反应。前列腺素E(2) (PGE(2)) 模拟了催产素对GnRH脉冲频率的刺激作用,抑制PG合成阻断了催产素的作用,表明催产素通过PGE(2) 加速了GnRH的脉冲释放。PGE(2) 的来源似乎是星形胶质细胞,因为催产素刺激PGE(2) 从培养的下丘脑星形胶质细胞释放。此外,星形胶质细胞表达催产素受体,而GnRH神经元不表达。这些结果表明,催产素促进了女性的性发育,并且这种作用是由涉及神经胶质产生的PGE(2) 的机制介导的。

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