首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Changes in brain testosterone and allopregnanolone biosynthesis elicit aggressive behavior.
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Changes in brain testosterone and allopregnanolone biosynthesis elicit aggressive behavior.

机译:脑睾丸激素和去甲泼尼龙的生物合成的变化引起攻击行为。

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In addition to an action on metabolism, anabolic/androgenic steroids also increase sex drive and mental acuity. If abused, such steroids can cause irritability, impulsive aggression, and signs of major depression [Pearson, H. (2004) Nature 431, 500-501], but the mechanisms that produce these symptoms are unknown. The present study investigates behavioral and neurochemical alterations occurring in association with protracted (3-week) administration of testosterone propionate (TP) to socially isolated (SI) and group-housed male and female mice. Male but not female SI mice exhibit aggression that correlates with the down-regulation of brain neurosteroid biosynthesis. However, in female mice, long-term TP administration induces aggression associated with a decrease of brain allopregnanolone (Allo) content and a decrease (approximately 40%) of 5alpha-reductase type I mRNA expression. In spayed mice treated with TP, restitution experiments with progesterone and estrogen normalize brain Allo content and prevent aggression. Submicromolar doses of S-norfluoxetine (S-NFLX) that are insufficient to inhibit serotonin reuptake selectively increase brain Allo content and abolish TP-induced aggression. Our results support the view that TP-induced aggressive behavior is the result of a TP-mediated neurosteroid biosynthesis down-regulation that can be reversed by the S-NFLX-induced increase of brain Allo content.
机译:除对新陈代谢有作用外,合成代谢/雄激素类固醇还增加性欲和智力。如果被滥用,这些类固醇会引起烦躁,冲动的侵略和严重抑郁的征兆[Pearson,H.(2004)Nature 431,500-501],但产生这些症状的机制尚不清楚。本研究调查了与社会隔离(SI)和成群饲养的雄性和雌性小鼠长期(3周)服用丙酸睾丸激素(TP)相关的行为和神经化学变化。雄性而非雌性SI小鼠表现出与大脑神经甾体生物合成的下调相关的攻击性。但是,在雌性小鼠中,长期TP给药会引起侵略性,其与大脑中Allallregnanolone(Allo)含量的降低和5α-还原酶I型mRNA表达的降低(约40%)有关。在接受TP处理的小白鼠中,用孕酮和雌激素进行的恢复实验可以使大脑中的Allo含量正常化并防止侵略。亚微摩尔剂量的S-诺氟西汀(S-NFLX)不足以抑制5-羟色胺的再摄取,有选择地增加了大脑的Allo含量并消除了TP引起的攻击。我们的结果支持以下观点:TP诱导的攻击行为是TP介导的神经类固醇生物合成下调的结果,该下调可以通过S-NFLX诱导的大脑同种异体含量的增加来逆转。

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