Early-life risperidone alters locomotor responses to apomorphine and quinpirole in adulthood

IF 2.6 3区 心理学 Q2 BEHAVIORAL SCIENCES Behavioural Brain Research Pub Date : 2024-07-31 DOI:10.1016/j.bbr.2024.115171
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Abstract

An escalating trend of antipsychotic drug use in children with ADHD, disruptive behavior disorder, or mood disorders has raised concerns about the impact of these drugs on brain development. Since antipsychotics chiefly target dopamine receptors, it is important to assay the function of these receptors after early-life antipsychotic administration. Using rats as a model, we examined the effects of early-life risperidone, the most prescribed antipsychotic drug in children, on locomotor responses to the dopamine D1/D2 receptor agonist, apomorphine, and the D2/D3 receptor agonist, quinpirole. Female and male Long-Evans rats received daily subcutaneous injections of risperidone (1.0 and 3.0 mg/kg) or vehicle from postnatal day 14–42. Locomotor responses to one of three doses (0.03, 0.1, and 0.3 mg/kg) of apomorphine or quinpirole were tested once a week for four weeks beginning on postnatal day 76 and 147 for each respective drug. The locomotor activity elicited by the two lower doses of apomorphine was significantly greater in adult rats, especially females, administered risperidone early in life. Adult rats administered risperidone early in life also showed more locomotor activity after the low dose of quinpirole. Overall, female rats were more sensitive to the locomotor effects of each agonist. In a separate group of rats administered risperidone early in life, autoradiography of forebrain D2 receptors at postnatal day 62 revealed a modest increase in D2 receptor density in the medial caudate. These results provide evidence that early-life risperidone administration can produce long-lasting changes in dopamine receptor function and density.

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早年的利培酮会改变成年后对阿扑吗啡和喹吡罗的运动反应。
患有多动症、破坏性行为障碍或情绪障碍的儿童使用抗精神病药物的趋势不断升级,这引起了人们对这些药物对大脑发育影响的关注。由于抗精神病药物主要以多巴胺受体为靶点,因此检测这些受体在早期服用抗精神病药物后的功能非常重要。我们以大鼠为模型,研究了儿童服用最多的抗精神病药物利培酮对多巴胺D1/D2受体激动剂阿朴吗啡和D2/D3受体激动剂喹吡罗的运动反应的影响。雌性和雄性Long-Evans大鼠在出生后第14-42天每天皮下注射利培酮(1.0和3.0毫克/千克)或药物。从大鼠出生后第 76 天和第 147 天开始,每周测试一次大鼠对三种剂量(0.03、0.1 和 0.3 毫克/千克)阿朴吗啡或喹吡罗中一种药物的运动反应,连续测试四周。成年大鼠(尤其是雌性大鼠)在出生后早期服用利培酮后,两种较低剂量的阿朴吗啡引起的运动活动明显增加。早期服用利培酮的成年大鼠在服用低剂量喹吡酮后也表现出更强的运动活性。总体而言,雌性大鼠对每种激动剂的运动效应都更为敏感。在另一组早期服用利培酮的大鼠中,出生后第62天前脑D2受体的自显影显示,内侧尾状核的D2受体密度略有增加。这些结果提供了证据,证明早期利培酮用药会对多巴胺受体的功能和密度产生持久的改变。
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来源期刊
Behavioural Brain Research
Behavioural Brain Research 医学-行为科学
CiteScore
5.60
自引率
0.00%
发文量
383
审稿时长
61 days
期刊介绍: Behavioural Brain Research is an international, interdisciplinary journal dedicated to the publication of articles in the field of behavioural neuroscience, broadly defined. Contributions from the entire range of disciplines that comprise the neurosciences, behavioural sciences or cognitive sciences are appropriate, as long as the goal is to delineate the neural mechanisms underlying behaviour. Thus, studies may range from neurophysiological, neuroanatomical, neurochemical or neuropharmacological analysis of brain-behaviour relations, including the use of molecular genetic or behavioural genetic approaches, to studies that involve the use of brain imaging techniques, to neuroethological studies. Reports of original research, of major methodological advances, or of novel conceptual approaches are all encouraged. The journal will also consider critical reviews on selected topics.
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