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Cocaine Self-Administration in Male and Female Rats Perinatally Exposed to PCBs: Evaluating Drug Use in an Animal Model of Environmental Contaminant Exposure

机译:可卡因自我管理在暴露于多氯联苯的雄性和雌性大鼠中:在环境污染动物模型中评估药物的使用

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摘要

Polychlorinated biphenyls (PCBs) are ubiquitous environmental toxicants known to adversely impact human health. Ortho-substituted PCBs affect the nervous system, including the brain dopaminergic system. The reinforcing effects of psychostimulants are typically modulated via the dopaminergic system, so this study used a preclinical (i.e., rodent) model to evaluate whether developmental contaminant exposure altered intravenous self-administration (i.v. SA) for the psychostimulant cocaine. Long Evans rats were perinatally exposed to 6 or 3 mg/kg/day of PCBs throughout gestation and lactation and compared to non-exposed controls. Rats were trained to lever press for a food reinforcer in an operant chamber under a fixed-ratio 5 (FR5) schedule and later underwent jugular catheterization. Food reinforcers were switched for infusions of 250 μg of cocaine, but the response requirement to earn the reinforcer remained. Active lever presses and infusions were higher in males during response acquisition and maintenance. The same sex effect was observed during later sessions which evaluated responding for cocaine doses ranging from 31.25 – 500 μg. PCB-exposed males (not females) exhibited an increase in cocaine infusions (with a similar trend in active lever presses) during acquisition, but no PCB-related differences were observed during maintenance, examination of the cocaine dose-response relationship, or progressive ratio sessions. Overall, these results indicated perinatal PCB exposure enhanced early cocaine drug-seeking in this preclinical model of developmental contaminant exposure (particularly the males), but no differences were seen during later cocaine SA sessions. As such, additional questions regarding substance abuse proclivity may be warranted in epidemiological studies evaluating environmental contaminant exposures.
机译:多氯联苯(PCB)是普遍存在的环境毒物,已知会对人体健康产生不利影响。邻位取代的多氯联苯会影响神经系统,包括脑多巴胺能系统。精神兴奋剂的增强作用通常是通过多巴胺能系统调节的,因此本研究使用临床前(即啮齿动物)模型评估发育污染物的暴露是否改变了精神兴奋剂可卡因的静脉内自我给药(i.v. SA)。在整个妊娠和哺乳期,长Evans大鼠在围产期暴露于6或3 mg / kg /天的PCB中,并与未暴露的对照组进行比较。对大鼠进行了训练,使其按照固定比例5(FR5)的时间表在手术室中压紧食物强化器,然后进行颈静脉导管插入术。更换了食品强化剂以输注250μg可卡因,但仍然需要获得强化剂的响应要求。在获得响应和维持响应期间,男性的主动杠杆按压和输注次数较高。在以后的疗程中观察到了相同的性效应,评估了可卡因剂量在31.25 – 500μg之间的反应。多氯联苯暴露的男性(非女性)在采集过程中可卡因输注量增加(主动杠杆按压趋势相似),但在维持,检查可卡因剂量反应关系或进行性比率过程中未观察到与多氯联苯相关的差异会议。总体而言,这些结果表明,在这种发展性污染物暴露的临床前模型(尤其是男性)中,围产期PCB暴露促进了早期可卡因药物的寻求,但在随后的可卡因SA疗程中未见差异。因此,在评估环境污染物暴露的流行病学研究中,可能还会有关于药物滥用倾向的其他问题。

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