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首页> 外文期刊>Behavioral neuroscience >Estradiol or Diarylpropionitrile Decrease Anxiety-Like Behavior of Wildtype, but Not Estrogen Receptor Beta Knockout, Mice
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Estradiol or Diarylpropionitrile Decrease Anxiety-Like Behavior of Wildtype, but Not Estrogen Receptor Beta Knockout, Mice

机译:雌二醇或二芳基丙腈降低野生型的焦虑行为,但不降低雌激素受体β基因敲除小鼠的行为

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摘要

Clinical and basic studies demonstrate that estrogen (E-2)-based therapies influence anxiety and mood. but the receptor targets (e.g., alpha or beta isoform of the estrogen receptor, ER) for these effects requires further investigation. To address the specificity of E-2's anxiolytic-like effects through ER beta, anxiety, motor, and nociceptive behavior of ovariectomized, wildtype (WT), and ER beta knockout (beta ERKO) mice was examined. Mice were administered oil vehicle or ER agonists, 17 beta-E-2 (E-2, 0.1 mg/kg: similar affinity for ER alpha and ER beta), and a selective ER modulator. diarylpropionitrile (DPN; 0. 1 mg/kg; greater affinity for ER beta than ER alpha). Performance of mice in anxiety (open field. elevated plus maze, elevated zero maze, social interaction), motor activity (activity monitor) and nociception (tailflick, pawlick) measures was compared. Results supported our hypothesis that ER beta is important in modulation of anxiety-like behavior by E, in some tasks. Administration of E-2 or DPN to WT, but not beta ERKO. mice increased open field central entries. plus maze open arm time, zero maze open quadrant time, and social interaction. This pattern was neither seen in motor activity nor pain threshold measures. Thus, actions of ER beta may be important for modulating anxiety-like behavior of mice.
机译:临床和基础研究表明,基于雌激素(E-2)的疗法会影响焦虑和情绪。但是针对这些作用的受体靶标(例如雌激素受体的ER或β异构体)需要进一步研究。为了解决E-2通过ERβ引起的抗焦虑样作用的特异性,检查了卵巢切除,野生型(WT)和ERβ敲除(βERKO)小鼠的焦虑,运动和伤害行为。给小鼠施用油溶媒或ER激动剂,17β-E-2(E-2,0.1mg / kg:对ERα和ERβ的相似亲和力)和选择性ER调节剂。二芳基丙腈(DPN; 0. 1 mg / kg;对ERβ的亲和力大于ERα)。比较了小鼠在焦虑(开阔地,高架迷宫,零迷宫升高,社交互动),运动活动(活动监测器)和伤害感受(tailflick,pawlick)措施下的表现。结果支持了我们的假设,即在某些任务中,ERβ对E调节焦虑样行为很重要。向WT管理E-2或DPN,但不向beta ERKO管理。小鼠增加了开放领域的中心条目。加上迷宫开放时间,零迷宫象限时间和社交互动。在运动活动和疼痛阈值测量中均未见该模式。因此,ERβ的作用对于调节小鼠的焦虑样行为可能很重要。

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