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雌激素可增加幼年和老年雌性恒河猴海马中亲棘蛋白免疫反应性棘突的数量。

Estrogen increases the number of spinophilin-immunoreactive spines in the hippocampus of young and aged female rhesus monkeys.

作者信息

Hao Jiandong, Janssen William G M, Tang Yong, Roberts Jeffrey A, McKay Heather, Lasley Bill, Allen Patrick B, Greengard Paul, Rapp Peter R, Kordower Jeffrey H, Hof Patrick R, Morrison John H

机构信息

Kastor Neurobiology of Aging Laboratories and Fishberg Research Center for Neurobiology, Mount Sinai School of Medicine, New York, New York 10029, USA.

出版信息

J Comp Neurol. 2003 Oct 27;465(4):540-50. doi: 10.1002/cne.10837.

Abstract

It is well documented that estrogen increases dendritic spine density in CA1 pyramidal cells of young female rats. However, this effect is attenuated in aged rats. We report here a quantitative analysis of estrogen effects on hippocampal spine number as visualized with antispinophilin in young (6-8 years old) and aged (19-23 years old) female rhesus monkeys, a species with a pattern of female endocrine senescence comparable to that of humans. Monkeys were ovariectomized and administered either vehicle or estradiol cypionate 3 months postovariectomy, followed by an additional dose 3 weeks later, with perfusion 24 hours after the last estrogen treatment. Immunolocalization of spinophilin, a spine-associated protein, was used for quantitative stereologic analyses of total spinophilin-immunoreactive spine numbers in CA1 stratum radiatum and the inner and outer molecular layers of dentate gyrus. In both young and aged female monkeys, the estrogen-treated groups had an increase in spinophilin-immunoreactive spines (37% in young, P <.005; 35% in aged, P <.05) compared with the untreated groups that amounted to more than 1 billion additional immunoreactive spines. The young group also showed a trend toward an estrogen-induced increase in immunoreactive spines in the dentate gyrus outer molecular layer, but this effect was not statistically significant (P =.097). We conclude that spine number in the rhesus monkey hippocampus is highly responsive to estrogen, yet, unlike the female rat, aged female rhesus monkeys retain the capacity for spine induction in response to estrogen. These data have important implications for cognitive effects of estrogen replacement in postmenopausal women and demonstrate that an estrogen replacement protocol that mimics normal physiological cycles with timed, intermittent peaks can have profound neurobiological effects.

摘要

有充分的文献记载,雌激素可增加幼年雌性大鼠海马CA1区锥体细胞的树突棘密度。然而,在老年大鼠中这种作用会减弱。我们在此报告一项对雌激素对幼年(6 - 8岁)和老年(19 - 23岁)雌性恒河猴海马棘突数量影响的定量分析,恒河猴的雌性内分泌衰老模式与人类相似。对猴子进行卵巢切除,在卵巢切除术后3个月给予溶剂或环丙孕酮酯,3周后再给予一剂,在最后一次雌激素治疗24小时后进行灌注。使用一种与棘突相关的蛋白亲棘蛋白的免疫定位法,对海马CA1辐射层以及齿状回内、外分子层中亲棘蛋白免疫反应性棘突的总数进行定量立体分析。与未治疗组相比,在幼年和老年雌性猴子中,雌激素治疗组的亲棘蛋白免疫反应性棘突均有所增加(幼年增加37%,P <.005;老年增加35%,P <.05),增加的免疫反应性棘突数量超过10亿个。幼年组在齿状回外分子层中也显示出雌激素诱导的免疫反应性棘突增加的趋势,但这种效应在统计学上不显著(P =.097)。我们得出结论,恒河猴海马中的棘突数量对雌激素高度敏感,然而,与雌性大鼠不同的是,老年雌性恒河猴保留了对雌激素诱导产生棘突的能力。这些数据对绝经后妇女雌激素替代的认知效应具有重要意义,并表明一种模拟正常生理周期、具有定时、间歇性峰值的雌激素替代方案可产生深远的神经生物学效应。

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