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首页> 外文期刊>Journal of psychopharmacology >Adult female wildtype, but not oestrogen receptor beta knockout, mice have decreased depression-like behaviour during pro-oestrus and following administration of oestradiol or diarylpropionitrile.
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Adult female wildtype, but not oestrogen receptor beta knockout, mice have decreased depression-like behaviour during pro-oestrus and following administration of oestradiol or diarylpropionitrile.

机译:成年雌性野生型小鼠,而不是雌激素受体β基因敲除小鼠,在发情期以及服用雌二醇或二芳基丙腈后,小鼠的抑郁样行为减少。

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Studies in people and animal models suggest that depression is influenced by natural fluctuations in the levels of 17beta-oestradiol (E(2)), as well as administration of E(2)-based therapies, such as selective oestrogen receptor modulators (SERMs). Elucidating the effects and mechanisms of E(2) is important to improve future E(2)-based therapeutics. An important question is whether effects of E(2) or SERMs for mood regulation act at the alpha or beta isoform of the oestrogen receptor (ER) because some of the unwanted trophic effects of E(2)-based therapies may involve actions at ERalpha, rather than ERbeta. In the present study, whether there are sex differences in depression-like behaviour of adult mice (experiment 1), and the effects of natural fluctuations in E(2) (experiment 2), or administration of E(2) or a SERM that has higher affinity for ERbeta than for ERalpha (diarylpropionitrile; DPN) to ovariectomised (experiment 3) wildtype and ERbeta knockout (betaERKO) mice were investigated. Results of this study supported our hypotheses that: there would be sex differences favouring males for depression-like behaviour and endogenous increases in, or exogenous administration of, E(2) or administration of an ERbeta SERM would decrease depression-like behaviour in wildtype, but not betaERKO, mice. In experiment 1, adult male mice spent less time immobile in the forced swim test (i.e., showed less depression-like behaviour) compared with female mice. In experiment 2, pro-oestrous (higher circulating E(2) levels), compared with dioestrous (lower circulating E(2) levels), mice had reduced immobility in the forced swim test; this effect was not observed in betaERKO mice. In experiment 3, administration of E(2) or DPN to ovariectomised wildtype, but not betaERKO, mice decreased immobility compared with vehicle administration, these data suggest that ERbeta may be required for some of the anti-depressant-like effects of E(2).
机译:在人和动物模型中的研究表明,抑郁症受17β-雌二醇(E(2))水平的自然波动以及基于E(2)的治疗方法(例如选择性雌激素受体调节剂(SERMs))的影响。阐明E(2)的作用和机制对于改善未来基于E(2)的疗法很重要。一个重要的问题是E(2)或SERM对情绪调节的作用是否作用于雌激素受体(ER)的α或β亚型,因为基于E(2)的疗法的某些不良营养作用可能涉及对ERalpha的作用,而不是ERbeta。在本研究中,成年小鼠的抑郁样行为是否存在性别差异(实验1),E(2)中自然波动的影响(实验2)或E(2)或SERM的使用与ERalpha(二芳基丙腈; DPN)相比,对ERbeta具有更高的亲和力。研究了去卵巢(实验3)野生型和ERbeta敲除(betaERKO)小鼠。这项研究的结果支持我们的假设:存在性别差异,有利于男性表现出抑郁症样的行为,内源性增加E(2)或外源施用E(2)或施用ERbeta SERM可以减少野生型的抑郁症样行为,但不是betaERKO,小鼠。在实验1中,与雌性小鼠相比,成年雄性小鼠在强迫游泳测试中花费的时间更少(即,表现出更少的抑郁样行为)。在实验2中,雌雄同体(较高的循环E(2)水平)与发情期(较低的循环E(2)水平)相比,小鼠在强迫游泳试验中的固定性降低;在betaERKO小鼠中未观察到这种作用。在实验3中,将E(2)或DPN给予卵巢切除的野生型,而非betaERKO,与媒介物给药相比,小鼠的固定性降低,这些数据表明ERbeta对于E(2)的某些抗抑郁样作用可能是必需的)。

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