Effect of progesterone on the activation of neurones of the supraoptic nucleus during parturition.

I A Antonijevic, J A Russell, R J Bicknell, G Leng, A J Douglas
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引用次数: 35

Abstract

Parturition is driven by a pulsatile pattern of oxytocin secretion, resulting from burst firing activity of supraoptic oxytocin neurones and reflected by induction of Fos expression. Rats were injected with progesterone on day 20 of pregnancy to investigate the role of the decreasing progesterone:ratio oestrogen ratio, which precedes delivery, in the activation of supraoptic neurones. Progesterone delayed the onset of birth by 28 h compared with vehicle (control) and prolonged the duration of delivery, which was overcome by pulsatile injections of oxytocin, indicating that the slow delivery may reflect impaired oxytocin secretion. Parturient rats pretreated with progesterone had fewer Fos immunoreactive nuclei in the supraoptic nucleus than did parturient rats pretreated with vehicle. The number of Fos immunoreactive nuclei was not restored after oxytocin injection, indicating that appropriate activation of oxytocin neurones is impaired by progesterone and also that there is a lack of stimulatory afferent drive. Fos expression increased in the nucleus of the tractus solitarius during parturition in rats pretreated with either vehicle or progesterone, but not in rats that had been pretreated with progesterone and induced with oxytocin, indicating that this input was inhibited. Endogenous opioids inhibit oxytocin neurones in late pregnancy and the opioid antagonist, naloxone, increases Fos expression in supraoptic nuclei by preventing inhibition. However, progesterone attenuated naloxone-induced Fos expression in the supraoptic nucleus in late pregnancy and naloxone administered during parturition did not accelerate the duration of births delayed by progesterone administration, indicating that progesterone does not act by hyperactivation of endogenous opioid tone. RU486, a progesterone receptor antagonist, enhanced supraoptic neurone Fos expression in late pregnancy, indicating progesterone receptor-mediated actions. Thus, progesterone withdrawal is necessary for appropriate activation of supraoptic and tractus solitarius neurones during parturition.

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孕酮对分娩时视上核神经元活化的影响。
分娩是由催产素分泌的脉动模式驱动的,由视上催产素神经元的突发放电活动引起,并通过诱导Fos表达来反映。大鼠在妊娠第20天注射黄体酮,观察分娩前黄体酮/雌激素比值降低对视上神经元激活的影响。与对照组相比,孕酮使分娩时间延迟28小时,分娩时间延长,但脉动注射催产素克服了这一障碍,表明分娩缓慢可能反映了催产素分泌受损。孕酮预处理大鼠视上核Fos免疫反应核数量少于胎鼠对照。注射催产素后Fos免疫反应核数量未恢复,提示孕激素损害了催产素神经元的正常激活,同时也缺乏刺激传入驱动。孕酮预处理和对照大鼠分娩时,孤束核Fos表达增加,孕酮预处理和催产素诱导的大鼠无Fos表达,表明Fos的输入受到抑制。内源性阿片样物质在妊娠后期抑制催产素神经元,阿片样物质拮抗剂纳洛酮通过防止抑制而增加视上核Fos的表达。然而,孕激素在妊娠后期减弱纳洛酮诱导的视上核Fos表达,分娩时给予纳洛酮并没有加速孕酮延迟的分娩时间,这表明孕酮不是通过内源性阿片张力的过度激活起作用的。孕激素受体拮抗剂RU486在妊娠后期增强视上神经元Fos的表达,提示孕激素受体介导的作用。因此,孕酮的戒断是必要的适当激活视上和孤束神经元在分娩期间。
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Characteristics and causes of the inadequate corpus luteum. Folliculogenesis in the sheep as influenced by breed, season and oestrous cycle. A changed responsiveness to oestrogen in ewes with clover disease. Nuclear transfer from somatic cells: applications in farm animal species. Identification and purification of inhibin and inhibin-related proteins.
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