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首页> 外文期刊>European neuropsychopharmacology: the journal of the European College of Neuropsychopharmacology >Attenuated disruption of prepulse inhibition by dopaminergic stimulation after maternal deprivation and adolescent corticosterone treatment in rats.
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Attenuated disruption of prepulse inhibition by dopaminergic stimulation after maternal deprivation and adolescent corticosterone treatment in rats.

机译:大鼠母体剥夺和青春期皮质酮治疗后,多巴胺能刺激减弱了对脉冲的抑制作用。

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The development of schizophrenia may include an early neurodevelopmental stress component which increases vulnerability to later stressful life events, in combination leading to overt disease. We investigated the effect of an early stress, in the form of maternal deprivation, combined with a later stress, simulated by chronic periadolescent corticosterone treatment, on behaviour in rats. Acute treatment with apomorphine caused disruption of prepulse inhibition (PPI) in controls and in rats that had undergone either maternal deprivation or corticosterone treatment, but was surprisingly absent in rats that had undergone the combined early and late stress. Amphetamine treatment significantly disrupted PPI in both non-deprived groups, but was absent in both maternally deprived groups. The serotonin-1A receptor agonist, 8-OH-DPAT, induced a significant disruption of PPI in all groups. Amphetamine-induced locomotor hyperactivity was similar in all groups. These results show an inhibitory interaction of earlystress, caused by maternal deprivation, combined with 'adolescent' stress, simulated by corticosterone treatment, on dopaminergic regulation of PPI. The altered effects of apomorphine and amphetamine could indicate differential changes in dopamine receptor signalling leading to functional desensitisation, or altered modulation of sensory gating in the nucleus accumbens by limbic structures such as the hippocampus.
机译:精神分裂症的发展可能包括早期的神经发育应激成分,该成分增加了对后期应激性生活事件的脆弱性,并导致明显的疾病。我们调查了早期应激(母体剥夺的形式)与后期应激(通过慢性青春期皮质激素治疗模拟)对大鼠行为的影响。阿朴吗啡的急性治疗可导致对照组和接受母体剥夺或皮质酮治疗的大鼠的前脉冲抑制(PPI)中断,但令人惊讶的是,其早,晚两种应激均未见。苯丙胺治疗在两个非贫困人群中均显着破坏PPI,但在两个母亲贫困人群中均不存在。血清素-1A受体激动剂8-OH-DPAT诱导所有组中的PPI显着破坏。在所有组中,苯丙胺诱导的运动亢进都相似。这些结果表明,由母体剥夺引起的早期应激与皮质酮治疗模拟的“青春期”应激对PPI的多巴胺能调节具有抑制作用。阿扑吗啡和苯丙胺的作用改变可能表明多巴胺受体信号传导的不同变化,导致功能性脱敏,或者伏隔核如海马体改变了伏隔核感觉门控的调节。

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