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年轻和老年雌性大鼠海马对雌激素反应的不同可塑性模式。

Different modes of hippocampal plasticity in response to estrogen in young and aged female rats.

作者信息

Adams M M, Shah R A, Janssen W G, Morrison J H

机构信息

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

出版信息

Proc Natl Acad Sci U S A. 2001 Jul 3;98(14):8071-6. doi: 10.1073/pnas.141215898. Epub 2001 Jun 26.

Abstract

Estrogen regulates hippocampal dendritic spine density and synapse number in an N-methyl-D-aspartate (NMDA) receptor-dependent manner, and these effects may be of particular importance in the context of age-related changes in endocrine status. We investigated estrogen's effects on axospinous synapse density and the synaptic distribution of the NMDA receptor subunit, NR1, within the context of aging. Although estrogen induced an increase in axospinous synapse density in young animals, it did not alter the synaptic representation of NR1, in that the amount of NR1 per synapse was equivalent across groups. Estrogen replacement in aged female rats failed to increase axospinous synapse density; however, estrogen up-regulated synaptic NR1 compared with aged animals with no estrogen. Therefore, the young and aged hippocampi react differently to estrogen replacement, with the aged animals unable to mount a plasticity response generating additional synapses, yet responsive to estrogen with respect to additional NMDA receptor content per synapse. These findings have important implications for estrogen replacement therapy in the context of aging.

摘要

雌激素以N-甲基-D-天冬氨酸(NMDA)受体依赖的方式调节海马树突棘密度和突触数量,并且在与年龄相关的内分泌状态变化的背景下,这些作用可能尤为重要。我们研究了在衰老背景下雌激素对轴棘突触密度和NMDA受体亚基NR1的突触分布的影响。虽然雌激素在幼龄动物中诱导轴棘突触密度增加,但它并未改变NR1的突触表现,因为每组中每个突触的NR1量是相等的。老年雌性大鼠的雌激素替代未能增加轴棘突触密度;然而,与未接受雌激素的老年动物相比,雌激素上调了突触NR1。因此,年轻和老年海马对雌激素替代的反应不同,老年动物无法产生可塑性反应以生成额外的突触,但对每个突触额外的NMDA受体含量对雌激素有反应。这些发现对衰老背景下的雌激素替代疗法具有重要意义。

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