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Early postnatal L-Dopa treatment causes behavioral alterations in female vs. male young adult Swiss mice

机译:早期产后L-DOPA治疗导致女性与男性年轻成人瑞士小鼠的行为改变

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Dopaminergic signaling and neurodevelopment alterations are associated with several neuropsychiatric disorders. Knockout mice for dopamine transporters (DAT) as well as site-specific knockout mice lacking dopaminergic D2 autoreceptors in dopaminergic neurons (DA-D2RKO) display behavioral alterations such as hyperlocomotion and abnormal prepulse inhibition. However, it is possible that dopaminergic imbalances may have different effects during varied neurodevelopmental windows. In our previous study, we observed that elevated levels of dopamine during the perinatal developmental window increased exploratory behavior of juvenile (4-week-old) Swiss female mice and impaired hedonic behavior in males. In this study, we investigated whether these behavioral alterations persist through young adulthood. In order to do so, we administered daily doses of L-Dopa to mice pups beginning from postnatal day 1 (PD1) to PD5. At the age of 8 weeks, we submitted the young adult males and females to the open field test, elevated plus maze, forced swimming test, and sucrose preference test. We observed that augmentation of dopamine levels during the perinatal developmental window increased locomotor behavior in females, but not males. We also observed an increase in anxiety-behavior in females and anxiolytic-like behavior in males. In addition, we observed stress-coping behavior in males and an increase of hedonic behavior in females. Our results show that dopamine signaling is important for behavioral development and that transient imbalances of dopamine levels can cause permanent behavioral alterations alterations which are different in males than in females. These data may help in better understanding the spectrum of symptoms associated with different neuropsychiatric disorders.
机译:多巴胺能信号和神经发育改变与几种神经精神障碍有关。多巴胺转运蛋白(DAT)的敲除小鼠以及在多巴胺能神经元(DA-D2RKO)中缺乏多巴胺能D2吸入器的特异性敲除小鼠(DA-D2RKO)显示行为改变,例如高冻伤和异常的预填种抑制。然而,多巴胺能失衡可能在不同的神经发育窗口期间具有不同的效果。在我们以前的研究中,我们观察到围产期发育窗口期间多巴胺水平提高了少年(4周龄)瑞士女性小鼠的探索性行为,并在雄性中受损的蜂窝行为。在这项研究中,我们调查了这些行为改变是否持续到年轻成年期。为此,我们将每日剂量的L-DOPA给小鼠幼仔从后期1(PD1)到PD5。在8周龄,我们将年轻的成年男性和女性提交到开放的现场测试,升高的迷宫,强制游泳试验和蔗糖偏好测试。我们观察到在围产期发育窗口期间增加多巴胺水平增加了女性的运动行为,但不是男性。我们还观察到女性和男性中抗焦虑行为的焦虑行为增加。此外,我们观察了男性的应力应对行为和女性中杂草行为的增加。我们的研究结果表明,多巴胺信号传导对行为发展至关重要,多巴胺水平的短暂性失衡可导致雄性不同的永久行为改变而不是女性。这些数据可能有助于更好地理解与不同神经精神障碍相关的症状的谱。

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