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首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >Early postnatal isolation reduces dopamine levels, elevates dopamine turnover and specifically disrupts prepulse inhibition in Nurr1-null heterozygous mice.
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Early postnatal isolation reduces dopamine levels, elevates dopamine turnover and specifically disrupts prepulse inhibition in Nurr1-null heterozygous mice.

机译:出生后早期隔离降低了多巴胺的水平,提高了多巴胺的转化率,并特别破坏了Nurr1无效的杂合小鼠的脉冲前抑制作用。

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Sensorimotor gating is a phenomenon that is linked with dopamine neurotransmission in limbic and cortical areas, and disruption of sensorimotor gating has been consistently demonstrated in schizophrenia patients. The nuclear receptor Nurr1 is essential for development of dopamine neurons and, using Nurr1-null heterozygous mice, has been found to be important for normal dopamine neurotransmission as null heterozygous mice have reduced limbic and cortical dopamine levels and elevated open-field locomotor activity. The current investigation compared sensorimotor gating, as measured by prepulse inhibition of the acoustic startle response, in Nurr1 wild-type and null heterozygous mice. When mice were weaned between 19 and 21 days of age either into isolation or groups of three to five and tested 12 weeks later, prepulse inhibition was elevated in group-raised null heterozygous mice and significantly disrupted in isolated null heterozygous mice as compared with isolation-raised wild-type mice and group-raised null heterozygous mice. Isolation had no effect on prepulse inhibition in wild-type mice. Isolation reduced tissue dopamine levels and elevated dopamine turnover in the nucleus accumbens and striatum in both wild-type and null heterozygous mice. In the prefrontal cortex, isolation reduced dopamine and 3,4-dihydroxyphenylacetic acid levels in null heterozygous as compared with isolation-raised wild-type mice, whereas no differences were observed between group-raised wild-type and null heterozygous mice. Neither the null heterozygous genotype nor isolation had any effect on basal or stress-induced corticosterone levels. These data suggest that the Nurr1 null heterozygous genotype predisposes these mice to isolation-induced disruption of prepulse inhibition that may be related to the interactions between intrinsic deficiencies in dopamine neurotransmission as a result of the null heterozygous genotype and isolation-induced changes in dopamine neurotransmission. Post-weaning isolation of Nurr1 null heterozygous mice provides a model to explore the interactions of genetic predisposition and environmenteurodevelopment on dopamine function that has important relevance to neuropsychiatric disorders.
机译:感觉运动门控是一种与边缘和皮质区域多巴胺神经传递有关的现象,并且在精神分裂症患者中始终证明感觉运动门控受到破坏。核受体Nurr1对多巴胺神经元的发育至关重要,并且使用Nurr1-null杂合子小鼠对正常的多巴胺神经传递很重要,因为无效的杂合子小鼠降低了边缘和皮质多巴胺水平,提高了开放运动能力。目前的研究在Nurr1野生型和无效杂合小鼠中比较了通过感觉惊吓反应的预脉冲抑制来测量的感觉运动门控。当小鼠在19至21日龄之间断奶进入隔离或三至五组时,并在12周后进行测试时,与隔离-饲养野生型小鼠和组饲养无效杂合小鼠。分离对野生型小鼠的前脉冲抑制没有影响。在野生型和无效杂合子小鼠中,分离降低伏隔核和纹状体中的组织多巴胺水平并提高多巴胺转换。与分离饲养的野生型小鼠相比,在前额叶皮层中,分离降低了无效杂合子中的多巴胺和3,4-二羟基苯基乙酸水平,而在组饲养的野生型和无效杂合子中没有观察到差异。无效的杂合基因型和分离都对基础或应激诱导的皮质酮水平没有任何影响。这些数据表明,Nurr1无效杂合基因型使这些小鼠易受隔离诱导的前脉冲抑制的破坏,这可能与无效杂合基因型和隔离诱导的多巴胺神经传递变化的结果导致的多巴胺神经传递固有缺陷之间的相互作用有关。断奶后分离的Nurr1空杂合小鼠提供了一个模型,用于探讨遗传易感性和环境/神经发育对多巴胺功能的相互作用,该作用与神经精神疾病具有重要的关系。

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