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用喹吡罗对新生大鼠进行处理后,其尼古丁致敏和条件性多动中的性别差异:D2和D3受体亚型的作用

Sex differences in nicotine sensitization and conditioned hyperactivity in adolescent rats neonatally treated with quinpirole: role of D2 and D3 receptor subtypes.

作者信息

Sheppard Brianna, Lehmann Julia, Cope Zackary A, Brown Russell W

机构信息

Department of Psychology, East Tennessee State University, Johnson City, TN 37614, USA.

出版信息

Behav Neurosci. 2009 Dec;123(6):1296-308. doi: 10.1037/a0017536.

Abstract

Neonatal quinpirole treatment in rats produces increased sensitivity of dopamine D2-like receptors throughout the animal's lifetime, referred to as D2 priming. There is little information on the effects of nicotine in adolescent rats, especially in a model that has clinical relevance to psychosis where increased D2 receptor sensitivity is common. Male and female rats were treated with quinpirole (1 mg/kg) or saline from postnatal (P) day 1-P21, given nicotine (0.5 mg/kg) or saline from P33 through P49, and placed into a locomotor arena for behavioral testing. Nicotine or saline treatment was preceded by the D2-like receptor antagonist eticlopride, D3 antagonist nafadotride, or saline. Conditioned hyperactivity was analyzed on P50 in the same context in a drug-free test. In females, D2 priming increased the locomotor response to acute nicotine, but did not affect subsequent nicotine sensitization, and only non-D2-primed females demonstrated conditioned hyperactivity. Eticlopride and nafadotride blocked behavioral sensitization, although nafadotride was more effective at blocking nicotine-conditioned hyperactivity in females. In males, D priming enhanced sensitization to nicotine and produced conditioned hyperactivity, which were blocked by eticlopride and nafadotride. These results have implications for psychosis and comorbidity of nicotine abuse in adolescence.

摘要

对大鼠进行新生期喹吡罗治疗会使其在整个生命周期内多巴胺D2样受体的敏感性增加,即所谓的D2致敏。关于尼古丁对青春期大鼠影响的信息很少,尤其是在与精神病具有临床相关性的模型中,其中D2受体敏感性增加很常见。从出生后(P)第1天至P21天,对雄性和雌性大鼠用喹吡罗(1毫克/千克)或生理盐水进行处理,从P33至P49天给予尼古丁(0.5毫克/千克)或生理盐水,然后将其放入运动场地进行行为测试。在给予尼古丁或生理盐水处理之前,先给予D2样受体拮抗剂依托必利、D3拮抗剂萘法唑酮或生理盐水。在P50天,在无药物的测试中,在相同环境下分析条件性多动。在雌性大鼠中,D2致敏增加了对急性尼古丁的运动反应,但不影响随后的尼古丁敏化,并且只有未进行D2致敏的雌性大鼠表现出条件性多动。依托必利和萘法唑酮阻断了行为敏化,尽管萘法唑酮在阻断雌性大鼠尼古丁条件性多动方面更有效。在雄性大鼠中,D致敏增强了对尼古丁的敏化并产生了条件性多动,这被依托必利和萘法唑酮阻断。这些结果对青春期精神病和尼古丁滥用合并症具有启示意义。

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