多靶点药物对雄性大鼠可卡因诱导的运动致敏表达的评估:一项比较研究。
Evaluation of multitarget drugs on the expression of cocaine-induced locomotor sensitization in male rats: A comparative study.
作者信息
Barbosa-Méndez Susana, Salazar-Juárez Alberto
机构信息
Subdirección de Investigaciones Clínicas. Laboratorio de Neurofarmacología Conductual, Microcirugía y Terapéutica Experimental. Instituto Nacional de Psiquiatría. Ciudad de México, 14370, Mexico.
出版信息
Heliyon. 2024 May 1;10(9):e29979. doi: 10.1016/j.heliyon.2024.e29979. eCollection 2024 May 15.
PURPOSE
- Cocaine use disorder (CUD) is a complex disease. Several studies have shown the efficacy of multitarget drugs used to treat CUD. Here we compare the efficacy of mirtazapine (MIR), pindolol (PIN), fluoxetine (FLX), risperidone (RIS), trazodone (TRZ), ziprasidone (ZPR), ondansetron (OND), yohimbine (YOH), or prazosin (PRZ), to reduce long-term cocaine-induced locomotor activity and the expression of cocaine-induced locomotor sensitization in rats.
METHODS
- The study consists of four experiments, which were divided into four experimental phases. Induction (10 days), cocaine withdrawal (30 days), expression (10 days), and post-expression phase (10 days). Male Wistar rats were daily dosed with cocaine (10 mg/kg; i.p.) during the induction and post-expression phases. During drug withdrawal, the MIR, PIN, FLX, RIS, TRZ, ZPR, OND, YOH, or PRZ were administered 30 min before saline. In the expression, the multitarget drugs were administered 30 min before cocaine. After each administration, locomotor activity for each animal was recorded for 30 min.During the agonism phase, in experiment four, 8-OH-DPAT, DOI, CP-809-101, SR-57227A, or clonidine (CLO) was administered 30 min before MIR and 60 min before cocaine. After each administration, locomotor activity for each animal was recorded for 30 min.
RESULTS
-MIR, FLX, RIS, ZPR, OND, or PRZ attenuated the cocaine-induced locomotor activity and cocaine locomotor sensitization. PIN, TRZ, and YOH failed to decrease cocaine locomotor sensitization. At the optimal doses used, PIN, FLX, RIS, TRZ, ZPR, OND, YOH, or PRZ failed to attenuate long-term cocaine locomotor activation. MIR generated a decrease in cocaine-induced locomotor activity of greater magnitude and duration than the other multitarget drugs evaluated.
CONCLUSION
- At the optimal doses of multitarget drugs evaluated, MIR was the multitarget drug that showed the greatest long-term cocaine-induced behavior effects compared to other multitarget drugs.
目的
可卡因使用障碍(CUD)是一种复杂的疾病。多项研究表明多靶点药物治疗CUD的疗效。在此,我们比较米氮平(MIR)、吲哚洛尔(PIN)、氟西汀(FLX)、利培酮(RIS)、曲唑酮(TRZ)、齐拉西酮(ZPR)、昂丹司琼(OND)、育亨宾(YOH)或哌唑嗪(PRZ)降低长期可卡因诱导的大鼠运动活性以及可卡因诱导的运动致敏表达的疗效。
方法
本研究包括四个实验,分为四个实验阶段。诱导期(10天)、可卡因戒断期(30天)、表达期(10天)和表达后期(10天)。雄性Wistar大鼠在诱导期和表达后期每天腹腔注射可卡因(10mg/kg)。在药物戒断期间,在注射生理盐水前30分钟给予MIR、PIN、FLX、RIS、TRZ、ZPR、OND、YOH或PRZ。在表达期,在注射可卡因前30分钟给予多靶点药物。每次给药后,记录每只动物30分钟的运动活性。在实验四的激动期,在给予MIR前30分钟和给予可卡因前60分钟给予8-OH-DPAT、DOI、CP-809-101、SR-57227A或可乐定(CLO)。每次给药后,记录每只动物30分钟的运动活性。
结果
MIR、FLX、RIS、ZPR、OND或PRZ减轻了可卡因诱导的运动活性和可卡因运动致敏。PIN、TRZ和YOH未能降低可卡因运动致敏。在所使用的最佳剂量下,PIN、FLX、RIS、TRZ、ZPR、OND、YOH或PRZ未能减轻长期可卡因运动激活。与其他评估的多靶点药物相比,MIR使可卡因诱导的运动活性降低的幅度和持续时间更大。
结论
在所评估的多靶点药物的最佳剂量下,与其他多靶点药物相比,MIR是显示出最大长期可卡因诱导行为效应的多靶点药物。
Zotero 插件