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雌激素缺乏增加三叉神经福尔马林模型中的疼痛:转基因ArKO小鼠的行为学和免疫细胞化学研究

Lack of estrogen increases pain in the trigeminal formalin model: a behavioural and immunocytochemical study of transgenic ArKO mice.

作者信息

Multon Sylvie, Pardutz Arpad, Mosen Jeanine, Hua Minh Tri, Defays Christian, Honda Shin-Ichiro, Harada Nobuhiro, Bohotin Catalina, Franzen Rachelle, Schoenen Jean

机构信息

Research Center for Cellular and Molecular Neurobiology, Neuroanatomy Laboratory, University of Liege, 4020 Liege, Belgium.

出版信息

Pain. 2005 Mar;114(1-2):257-65. doi: 10.1016/j.pain.2004.12.030. Epub 2005 Jan 26.

Abstract

In order to examine the effect of estrogen on facial pain, we first compared the face-rubbing evoked by a formalin injection in the lip of aromatase-knockout (ArKO) mice, lacking endogenous estrogen production, 17 beta-estradiol-treated ArKO mice (ArKO-E2) and wild-type (WT) littermates. During the 'acute' phase of pain the time spent rubbing was similar in the three groups, whereas during the following 'interphase' and the second phase of pain, grooming was increased in ArKO mice. Estradiol-treatment restored a behaviour similar to WT group. To better understand estrogens modulation on pain processes, we examined changes in 5-HT and CGRP innervations of trigeminal nucleus caudalis (TNC) in ArKO, ArKO-E2 and WT groups sacrificed during the interphase. Whereas serotonin and CGRP immunoreactivities were comparable in WT and ArKO non-injected control groups, our data showed that 9 min after formalin injection, the density of serotoninergic terminals increased significantly in WT, but not in ArKO mice, while that of CGRP-immunoreactive fibers was lower in WT than in ArKO mice on the injected side. Estradiol-treatment only partially reversed these changes in ArKO-E2 mice. We conclude that estrogen deprivation in ArKO mice can be responsible for increased nociceptive response and that it is accompanied by transmitter changes favouring pro- over anti-nociceptive mechanisms in TNC during interphase of the formalin model. That estradiol-treatment completely reverses the behavioural abnormality suggests that estrogens absence produces chiefly functional activation-dependent changes. However, the fact that the immunohistochemical abnormalities were not totally normalized by estradiol-treatment suggested that some permanent developmental alterations may occur in ArKO mice.

摘要

为了研究雌激素对面部疼痛的影响,我们首先比较了芳香化酶基因敲除(ArKO)小鼠(缺乏内源性雌激素产生)、经17β-雌二醇处理的ArKO小鼠(ArKO-E2)和野生型(WT)同窝小鼠在唇部注射福尔马林后诱发的擦脸行为。在疼痛的“急性期”,三组小鼠擦脸的时间相似,而在随后的“间期”和疼痛的第二阶段,ArKO小鼠的梳理行为增加。雌二醇处理恢复了与WT组相似的行为。为了更好地理解雌激素对疼痛过程的调节作用,我们检查了在间期处死的ArKO、ArKO-E2和WT组小鼠三叉神经尾核(TNC)中5-羟色胺(5-HT)和降钙素基因相关肽(CGRP)神经支配的变化。虽然在WT和未注射福尔马林的ArKO对照组中,5-羟色胺和CGRP免疫反应性相当,但我们的数据显示,福尔马林注射9分钟后,WT小鼠中5-羟色胺能终末的密度显著增加,而ArKO小鼠中则没有,并且在注射侧,WT小鼠中CGRP免疫反应性纤维的密度低于ArKO小鼠。雌二醇处理仅部分逆转了ArKO-E2小鼠中的这些变化。我们得出结论,ArKO小鼠中的雌激素缺乏可能导致伤害性反应增加,并且在福尔马林模型的间期,它伴随着TNC中有利于促伤害性而非抗伤害性机制的递质变化。雌二醇处理完全逆转行为异常这一事实表明,雌激素缺乏主要产生功能激活依赖性变化。然而,免疫组织化学异常未被雌二醇处理完全归一化这一事实表明,ArKO小鼠中可能发生了一些永久性的发育改变。

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