社会孤立诱发性别攻击的脑神经类固醇

Graziano Pinna, Roberto C Agis-Balboa, Mohemed-Salim Doueiri, Alessandro Guidotti, Erminio Costa
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引用次数: 45

摘要

遗传、环境或激素因素及其相互作用与人类性别相关攻击行为的表达有关。几条独立的证据线支持激素和环境因素在实验动物的攻击行为中的作用。社会隔离(SI)在雄性小鼠中持续2-4周,而在雌性小鼠中没有,结果对同性入侵者表现出攻击性。在社会隔离(SI)期间,雌性小鼠长期使用合成代谢类固醇治疗(3周)会诱导对雄性入侵者的攻击行为,其严重程度与在社会隔离(SI)雄性小鼠中观察到的相似。雄性和雌性小鼠的诱导攻击与脑内异丙孕酮(Allo)的减少有关。在SI雄性小鼠中,用l -蛋氨酸(MET)治疗可以预防攻击行为,这也被证明可以降低reelin和GAD67 mRNA的表达并维持正常的脑Allo含量。组蛋白去乙酰化酶抑制剂丙戊酸可以逆转这一过程,提示组蛋白尾部乙酰化可能逆转MET的作用。我们得出结论,在社会隔离期间,攻击可以通过防止Allo下调(例如,通过MET治疗)或通过直接施用Allo或上调SI小鼠脑Allo含量的药物(例如氟西汀)来控制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Brain neurosteroids in gender-related aggression induced by social isolation.

Genetic, environmental, or hormonal factors and their interactions have been implicated in the expression of gender-related aggressive behavior in humans. Several independent lines of evidence support the role of hormonal and environmental factors in the aggressive behavior of experimental animals. Social isolation (SI) for 2-4 weeks in male but not in female mice results in the expression of aggression to a same-sex intruder. Long-term treatment (3 weeks) with anabolic steroids during SI in female mice induces aggressive behavior toward a male intruder of a severity similar to that observed in socially isolated (SI) male mice. The induced aggression in male and female mice is associated with a decrease of brain allopreg-nanolone (Allo). In SI male mice, aggression can be prevented by treatment with L-methionine (MET), which has also been shown to decrease reelin and GAD67 mRNA expression and maintain normal brain Allo content. The histone deacetylase inhibitor valproic acid can reverse this process, suggesting that histone tail acetylation may reverse the action of MET. We conclude that during social isolation, aggression can be controlled either by preventing Allo downregulation (e.g., by treatment with MET) or by direct administration of Allo or of agents (e.g., fluoxetine) that upregulate brain Allo content in SI mice.

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