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胰岛素替代可恢复链脲佐菌素处理大鼠中喹吡罗和雷氯必利的行为效应。

Insulin replacement restores the behavioral effects of quinpirole and raclopride in streptozotocin-treated rats.

作者信息

Sevak Rajkumar J, Koek Wouter, Galli Aurelio, France Charles P

机构信息

Department of Pharmacology, The University of Texas Health Science Center at San Antonio, San Antonio, TX 78229, USA.

出版信息

J Pharmacol Exp Ther. 2007 Mar;320(3):1216-23. doi: 10.1124/jpet.106.115600. Epub 2006 Dec 14.

Abstract

Streptozotocin (STZ)-induced diabetes can modulate dopamine (DA) neurotransmission and thereby modify the behavioral effects of drugs acting on DA systems. Insulin replacement, and in some conditions repeated treatment with amphetamine, can partially restore sensitivity of STZ-treated rats to dopaminergic drugs. The present study sought to characterize the role of insulin and amphetamine in modulating the behavioral effects of drugs that selectively act on D2/D3 receptors. In control rats, quinpirole and quinelorane produced yawning, whereas raclopride and gamma-hydroxybutyric acid (GHB) produced catalepsy. Raclopride antagonized quinpirole- and quinelorane-induced yawning with similar potency. STZ treatment increased blood glucose concentration, decreased body weight, and markedly reduced sensitivity to quinpirole-induced yawning, quinelorane-induced yawning as well as to raclopride-induced catalepsy, while enhancing sensitivity to GHB-induced catalepsy. Repeated treatment with amphetamine partially restored sensitivity of STZ-treated rats to amphetamine-stimulated locomotion and also produced conditioned place preference, without affecting blood glucose and body weight changes. However, amphetamine treatment did not restore sensitivity to the behavioral effects of quinpirole, raclopride, or GHB, suggesting differential regulation of dopamine transporter activity and sensitivity of D2 receptors in hypoinsulinemic rats. Insulin replacement in STZ-treated rats normalized blood glucose and body weight changes and fully restored sensitivity to quinpirole-induced yawning, as well as to raclopride-induced catalepsy, while reducing sensitivity to GHB-induced catalepsy. Overall, these data indicate that changes in insulin status markedly affect sensitivity to the behavioral effects of dopaminergic drugs. The results underscore the importance of insulin in modulating DA neurotransmission; these effects might be especially relevant to understanding the co-morbidity of eating disorders and substance abuse.

摘要

链脲佐菌素(STZ)诱导的糖尿病可调节多巴胺(DA)神经传递,从而改变作用于DA系统的药物的行为效应。胰岛素替代治疗,以及在某些情况下用苯丙胺重复治疗,可部分恢复STZ处理大鼠对多巴胺能药物的敏感性。本研究旨在表征胰岛素和苯丙胺在调节选择性作用于D2/D3受体的药物行为效应中的作用。在对照大鼠中,喹吡罗和喹氯雷司可引起打哈欠,而雷氯必利和γ-羟基丁酸(GHB)可引起僵住。雷氯必利以相似的效力拮抗喹吡罗和喹氯雷司诱导的打哈欠。STZ处理可提高血糖浓度、降低体重,并显著降低对喹吡罗诱导的打哈欠、喹氯雷司诱导的打哈欠以及雷氯必利诱导的僵住的敏感性,同时增强对GHB诱导的僵住的敏感性。用苯丙胺重复治疗可部分恢复STZ处理大鼠对苯丙胺刺激的运动的敏感性,还可产生条件性位置偏爱,而不影响血糖和体重变化。然而,苯丙胺治疗并未恢复对喹吡罗、雷氯必利或GHB行为效应的敏感性,提示低胰岛素血症大鼠中多巴胺转运体活性和D2受体敏感性的调节存在差异。对STZ处理大鼠进行胰岛素替代可使血糖和体重变化正常化,并完全恢复对喹吡罗诱导的打哈欠以及雷氯必利诱导的僵住的敏感性,同时降低对GHB诱导的僵住的敏感性。总体而言,这些数据表明胰岛素状态的变化显著影响对多巴胺能药物行为效应的敏感性。结果强调了胰岛素在调节DA神经传递中的重要性;这些效应可能与理解饮食失调和药物滥用的共病情况特别相关。

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