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trkA神经生长因子受体在哺乳动物排卵中的作用。

A role for trkA nerve growth factor receptors in mammalian ovulation.

作者信息

Dissen G A, Hill D F, Costa M E, Les Dees C W, Lara H E, Ojeda S R

机构信息

Division of Neuroscience, Oregon Regional Primate Research Center/Oregon Health Sciences University, Beaverton 97006-3499, USA.

出版信息

Endocrinology. 1996 Jan;137(1):198-209. doi: 10.1210/endo.137.1.8536613.

Abstract

Several members of the neurotrophin (NT) family, including nerve growth factor (NGF), NT-3, and NT-4/5, are expressed in the mammalian ovary. As their respective receptor tyrosine kinases are also found in the gland, the possibility exists that NTs act directly on the gonads to exert effects unrelated to their support of the ovarian innervation. We now report that trkA, the NGF receptor tyrosine kinase, is involved in the acute activational process that leads to the first ovulation. The trkA gene becomes transiently expressed in periovulatory follicules at the time of the first preovulatory surge of gonadotropins at puberty; the increase in trkA messenger RNA (mRNA) content is dramatic ( > 100-fold), but transient (approximately 9 h). No such changes in trkB or trkC mRNA were observed; the abundance of these mRNAs, which encode the receptor tyrosine kinase for NT-4/5 and brain-derived neurotrophic factor, and NT-3, respectively, remained at very low levels throughout puberty. In vivo and in vitro experiments demonstrated that the activation of trkA gene expression is brought about by the proestrous discharge of LH. The increase in trkA mRNA levels is mainly localised to cells of the follicular wall and interstitial tissue of the ovary. NGF mRNA abundance also increases at proestrus, with peak values detected about 5 h before ovulation; as in the case of trkA mRNA, NGF mRNA was found in thecal-interstitial cells. Both trkA and NGF protein, detected by immunohistochemistry, were localized to this same ovarian compartment. Interleukin-1 beta (IL-1 beta), a putative mediator of LH action, enhances both trkA and NGF gene expression in ovarian cells, an effect prevented by IL-1ra, a natural IL-1 beta receptor antagonist. Il-1 beta also stimulates PGE2 release, and this effect was inhibited by both NGF antibodies and a trk receptor blocker, NGF antibodies administered in vivo attenuated the increase in ovarian PGE2 synthesis that antedates ovulation. Immunoneutralization of NGF action or pharmacological blockade of trk tyrosine kinase activity targeted to one ovary resulted in the ipsilateral inhibition of ovulation. The remarkably narrow time frame of trkA gene activation at the completion of follicular growth suggests that NGF acting as a neuroendocrinotrophic factor in a developmentally restricted manner contributes to the acute cytodifferentiation process that leads to the first ovulation in mammals.

摘要

神经营养因子(NT)家族的多个成员,包括神经生长因子(NGF)、NT-3和NT-4/5,在哺乳动物卵巢中表达。由于在该腺体中也发现了它们各自的受体酪氨酸激酶,因此存在NTs直接作用于性腺以发挥与其对卵巢神经支配的支持无关的作用的可能性。我们现在报告,NGF受体酪氨酸激酶trkA参与了导致首次排卵的急性激活过程。trkA基因在青春期促性腺激素首次排卵前激增时,在排卵前卵泡中短暂表达;trkA信使核糖核酸(mRNA)含量的增加非常显著(>100倍),但很短暂(约9小时)。未观察到trkB或trkC mRNA有此类变化;这些分别编码NT-4/5和脑源性神经营养因子以及NT-3的受体酪氨酸激酶的mRNA丰度在整个青春期都维持在非常低的水平。体内和体外实验表明,trkA基因表达的激活是由LH的动情前期释放引起的。trkA mRNA水平的增加主要定位于卵巢卵泡壁和间质组织的细胞。NGF mRNA丰度在动情前期也增加,在排卵前约5小时检测到峰值;与trkA mRNA的情况一样,在卵泡膜间质细胞中发现了NGF mRNA。通过免疫组织化学检测到的trkA和NGF蛋白都定位于卵巢的同一区域。白细胞介素-1β(IL-1β)是LH作用的一种假定介质,可增强卵巢细胞中trkA和NGF基因的表达,天然IL-1β受体拮抗剂IL-1ra可阻止这种作用。IL-1β还刺激PGE2释放,NGF抗体和trk受体阻滞剂均可抑制这种作用,体内注射NGF抗体可减弱排卵前卵巢PGE2合成的增加。针对一侧卵巢的NGF作用的免疫中和或trk酪氨酸激酶活性的药理学阻断导致同侧排卵受到抑制。卵泡生长完成时trkA基因激活的时间框架非常狭窄,这表明NGF作为一种以发育受限方式起作用的神经内分泌营养因子,有助于导致哺乳动物首次排卵的急性细胞分化过程。

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