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哺乳动物卵巢神经元的起源与个体发生。

Origin and ontogeny of mammalian ovarian neurons.

作者信息

Dees W Les, Hiney J K, McArthur N H, Johnson G A, Dissen G A, Ojeda S R

机构信息

Department of Veterinary Integrative Biosciences, College of Veterinary Medicine, Texas A&M University, College Station, Texas 77845-4458, USA.

出版信息

Endocrinology. 2006 Aug;147(8):3789-96. doi: 10.1210/en.2006-0394. Epub 2006 May 25.

Abstract

Mammalian ovaries contain sympathetic neurons expressing the low affinity neurotropin receptor (p75NTR). To date neither the role these neurons might play in ovarian physiology nor their embryological origin is known. Immunohistochemistry was used to detect postnatal changes in distribution and number of both p75NTR-positive and tyrosine hydroxylase-positive neurons in rhesus monkey ovaries. Pig fetuses were used to map the pathway of ovarian neuronal migration during embryonic development. Antiserum to p75NTR revealed the presence of isolated neurons and neurons clustered into ganglia in 2-month-old monkey ovaries. After 8 months, the neurons exhibited well-developed processes, and other than being more extensively interlaced, the localization and morphology did not change after 2 yr of age. Total number of p75NTR-positive neurons present decreased gradually between 2 months and 12 yr of age and declined markedly with reproductive aging. Conversely, the subpopulation of neurons immunoreactive to anti-tyrosine hydroxylase increased significantly at puberty and then declined with the loss of reproductive capacity. By d 21 of fetal life in the pig, p75NTR neurons had migrated medially from the neural crest to form the paraaortic autonomic ganglia. Some neurons migrated ventrally from the ganglia and then continued ventrolaterally to enter the genital ridge. By d 27, neurons had entered the developing ovary, and by d 35, the migration was complete with neurons demonstrating immunoreactivity to NeuN, a neuron-specific marker. Results demonstrate that p75NTR-expressing ovarian neurons originate from the neural crest and that a catecholaminergic subset is associated with pubertal maturation of the ovary and subsequent reproductive function.

摘要

哺乳动物的卵巢含有表达低亲和力神经营养因子受体(p75NTR)的交感神经元。迄今为止,这些神经元在卵巢生理学中可能发挥的作用及其胚胎起源均不明确。采用免疫组织化学方法检测恒河猴卵巢中p75NTR阳性神经元和酪氨酸羟化酶阳性神经元在出生后的分布及数量变化。利用猪胎儿来绘制胚胎发育过程中卵巢神经元的迁移路径。抗p75NTR抗血清显示,2月龄猴卵巢中存在孤立的神经元和聚集成神经节的神经元。8个月后,神经元表现出发育良好的突起,除了相互交织更为广泛外,2岁后其定位和形态没有变化。2月龄至12岁之间,p75NTR阳性神经元的总数逐渐减少,并随着生殖衰老而显著下降。相反,对抗酪氨酸羟化酶免疫反应的神经元亚群在青春期显著增加,然后随着生殖能力的丧失而下降。在猪胎儿生命的第21天,p75NTR神经元已从神经嵴向内侧迁移,形成主动脉旁自主神经节。一些神经元从神经节向腹侧迁移,然后继续向腹外侧迁移进入生殖嵴。到第27天,神经元已进入发育中的卵巢,到第35天,迁移完成,神经元对神经元特异性标志物NeuN呈免疫反应。结果表明,表达p75NTR的卵巢神经元起源于神经嵴,并且一个儿茶酚胺能亚群与卵巢的青春期成熟及随后的生殖功能相关。

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