首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Serotonin and arginine–vasopressin mediate sex differences in the regulation of dominance and aggression by the social brain
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Serotonin and arginine–vasopressin mediate sex differences in the regulation of dominance and aggression by the social brain

机译:5-羟色胺和精氨酸加压素介导性别差异调节社交大脑的支配性和攻击性

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摘要

There are profound sex differences in the incidence of many psychiatric disorders. Although these disorders are frequently linked to social stress and to deficits in social engagement, little is known about sex differences in the neural mechanisms that underlie these phenomena. Phenotypes characterized by dominance, competitive aggression, and active coping strategies appear to be more resilient to psychiatric disorders such as posttraumatic stress disorder (PTSD) compared with those characterized by subordinate status and the lack of aggressiveness. Here, we report that serotonin (5-HT) and arginine–vasopressin (AVP) act in opposite ways in the hypothalamus to regulate dominance and aggression in females and males. Hypothalamic injection of a 5-HT1a agonist stimulated aggression in female hamsters and inhibited aggression in males, whereas injection of AVP inhibited aggression in females and stimulated aggression in males. Striking sex differences were also identified in the neural mechanisms regulating dominance. Acquisition of dominance was associated with activation of 5-HT neurons within the dorsal raphe in females and activation of hypothalamic AVP neurons in males. These data strongly indicate that there are fundamental sex differences in the neural regulation of dominance and aggression. Further, because systemically administered fluoxetine increased aggression in females and substantially reduced aggression in males, there may be substantial gender differences in the clinical efficacy of commonly prescribed 5-HT–active drugs such as selective 5-HT reuptake inhibitors. These data suggest that the treatment of psychiatric disorders such as PTSD may be more effective with the use of 5-HT–targeted drugs in females and AVP-targeted drugs in males.
机译:在许多精神疾病的发病率中存在深远的性别差异。尽管这些疾病经常与社会压力和社会参与不足有关,但对于造成这些现象的神经机制的性别差异知之甚少。与那些以从属地位和缺乏攻击性为特征的表型相比,以优势性,竞争性攻击和积极应对策略为特征的表型似乎对诸如创伤后应激障碍(PTSD)之类的精神疾病具有更强的适应力。在这里,我们报道5-羟色胺(5-HT)和精氨酸-加压素(AVP)在下丘脑中以相反的方式调节雌性和雄性的优势和侵略性。下丘脑注射5-HT1a激动剂可刺激雌性仓鼠的侵略性并抑制雄性的侵略,而注射AVP则可抑制雌性仓鼠的侵害性并刺激雄性的侵略性。在调节优势的神经机制中也发现了惊人的性别差异。在女性中,获得支配地位与背背沟内的5-HT神经元活化以及在男性中激活下丘脑AVP神经元有关。这些数据强烈表明,在支配性和攻击性的神经调节中存在根本的性别差异。此外,由于全身使用氟西汀会增加女性的攻击性,而男性的攻击性会大大降低,因此通常处方的5-HT活性药物(例如选择性5-HT再摄取抑制剂)的临床疗效可能存在明显的性别差异。这些数据表明,女性使用5-HT靶向药物,男性使用AVP靶向药物,对精神疾病如PTSD的治疗可能更有效。

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