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雌激素和穹窿/穹窿海马伞横断对布罗卡内侧隔核和斜角带中p75神经营养因子受体(p75NGFR)和胆碱乙酰转移酶(ChAT)表达的影响

Effects of estrogen and fimbria/fornix transection on p75NGFR and ChAT expression in the medial septum and diagonal band of Broca.

作者信息

Gibbs R B, Pfaff D W

机构信息

Laboratory of Neurobiology and Behavior, The Rockefeller University, 1230 York Avenue, New York, New York 10021.

出版信息

Exp Neurol. 1992 Apr;116(1):23-39. doi: 10.1016/0014-4886(92)90173-n.

Abstract

NGF receptor-expressing cells located in the basal forebrain have recently been shown to contain estrogen (E) receptors (Toran-Allerand and MacLusky. 1989. Soc. Neurosci. Abstr. 15: 954). In the present study, we have examined the effects of E-treatment on p75NGFR and choline acetyltransferase (ChAT) expression by neurons in the medial septum (MS) and the vertical (VDB) and horizontal (HDB) limbs of the diagonal band of Broca using immunocytochemical and in situ hybridization techniques. First, since E-treatment has been shown to affect neuronal survival and to stimulate synaptic reorganization and growth within various regions of the brain, we hypothesized that E-treatment might attenuate the loss of p75NGFR immunoreactivity (IR) which occurs in the MS and VDB following transection of the fimbria/fornix. Contrary to our hypothesis, E-treatment did not attenuate the effects of fimbria/fornix transection. In fact, E-treatment alone produced a significant decrease in the number of p75NGFR-IR cells detected in the MS. Subsequent experiments confirmed that chronic E-treatment produces a down-regulation of both p75NGFR-IR and p75NGFR mRNA in the MS and VDB. In the MS, estrogen appeared to affect a subpopulation of p75NGFR-expressing neurons which were also affected by fimbria/fornix transection since the effects of these two treatments were not additive. In addition, effects of E-treatment on p75NGFR-IR were sex-specific (observed in females but not in males) and were reversible in the MS after 2 weeks, but not after 4 weeks (allowing 2 weeks recovery), of E-treatment. A time-course analysis revealed that effects of E-treatment on p75NGFR-IR were not observed until after 16 days (MS) or 30 days (VDB) of E-treatment and were preceded by a significant and transient increase in ChAT expression in both the MS and VDB. The data are consistent with the possibility that continuous, long-term exposure to gonadal steroids may contribute to a loss of p75NGFR-expressing neurons with age. In addition, the data suggest that p75NGFR expression may play a role in regulating the functioning of specific basal forebrain cholinergic neurons. Different mechanisms by which E-treatment might influence ChAT and p75NGFR expression in brain are discussed.

摘要

最近研究表明,位于基底前脑表达神经生长因子(NGF)受体的细胞含有雌激素(E)受体(托兰 - 阿兰德和麦克卢斯基,1989年,神经科学学会摘要15:954)。在本研究中,我们使用免疫细胞化学和原位杂交技术,研究了雌激素处理对内侧隔区(MS)以及布罗卡斜带垂直部(VDB)和水平部(HDB)中神经元的p75NGFR和胆碱乙酰转移酶(ChAT)表达的影响。首先,由于已证明雌激素处理会影响神经元存活,并刺激大脑各区域内的突触重组和生长,我们推测雌激素处理可能会减弱在穹窿/穹窿海马伞横断后内侧隔区和VDB中发生的p75NGFR免疫反应性(IR)丧失。与我们的假设相反,雌激素处理并未减弱穹窿/穹窿海马伞横断的影响。事实上,单独的雌激素处理使在内侧隔区检测到的p75NGFR-IR细胞数量显著减少。后续实验证实,长期雌激素处理会导致内侧隔区和VDB中p75NGFR-IR和p75NGFR mRNA的下调。在内侧隔区中,雌激素似乎影响了表达p75NGFR的神经元亚群,这些神经元也受到穹窿/穹窿海马伞横断的影响,因为这两种处理的效果并非相加。此外,雌激素处理对p75NGFR-IR的影响具有性别特异性(在雌性中观察到,而在雄性中未观察到),并且在内侧隔区中,雌激素处理2周后(允许2周恢复)影响是可逆的,但4周后则不可逆。时间进程分析表明,直到雌激素处理16天(内侧隔区)或30天(VDB)后才观察到雌激素处理对p75NGFR-IR的影响,并且在此之前内侧隔区和VDB中ChAT表达均有显著且短暂的增加。这些数据与长期持续暴露于性腺类固醇可能导致随着年龄增长表达p75NGFR的神经元丧失的可能性一致。此外,数据表明p75NGFR表达可能在调节特定基底前脑胆碱能神经元的功能中起作用。本文讨论了雌激素处理可能影响大脑中ChAT和p75NGFR表达的不同机制。

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