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Efficacy of an Adenovirus-based Anti-cocaine Vaccine to Reduce Cocaine Self-administration and Reacqusition using a Choice Procedure in Rhesus Macaques

机译:基于腺病毒的抗可卡因疫苗减少猕猴的可卡因自我管理和使用选择程序的重新获得的功效。

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摘要

Immunopharmacotherapy offers an approach for treating cocaine abuse by specifically targeting the cocaine molecule and preventing its access to the CNS. dAd5GNE is a novel cocaine vaccine that attenuates the stimulant and the reinforcing effects of cocaine in rats. The goal of this study was to extend and validate dAd5GNE vaccine efficacy in non-human primates. Six experimentally naïve adult female rhesus monkeys (Macaca mulatta) were trained to self-administer 0.1 mg/kg/injection intravenous (i.v.) cocaine or receive candy; then 4 monkeys were administered the vaccine and 2 monkeys were administered vehicle intramuscularly, with additional vaccine boosts throughout the study. The reinforcing effects of cocaine were measured during self-administration, extinction, and reacquisition (relapse) phases. Serum antibody titers in the vaccinated monkeys remained high throughout the study. There was no change in the preference for cocaine over candy over a 20-week period in 5 of the 6 monkeys; only one of the 4 (25%) vaccinated monkeys showed a decrease in cocaine choice. All 6 monkeys extinguished responding for cocaine during saline extinction testing; vaccinated monkeys tended to take longer to extinguish responding than control monkeys (17.5 vs. 7.0 sessions). Vaccination substantially retarded reacquisition of cocaine self-administration; control monkeys resumed cocaine self-administration within 6–41 sessions and 1 vaccinated monkey resumed cocaine self-administration in 19 sessions. The other 3 vaccinated monkeys required between 57–94 sessions to resume cocaine self-administration even in the context of employing several manipulations to encourage cocaine reacquisition. These data suggest that the dAdGNE vaccine may have therapeutic potential for humans who achieve cocaine abstinence as part of a relapse prevention strategy.
机译:免疫药物疗法通过专门针对可卡因分子并阻止其进入中枢神经系统提供了一种治疗可卡因滥用的方法。 dAd5GNE是一种新型可卡因疫苗,可减轻可卡因对大鼠的刺激作用和增强作用。这项研究的目的是扩展和验证dAd5GNE疫苗在非人类灵长类动物中的功效。训练了六只实验性幼稚的成年雌性恒河猴(猕猴)自行施用0.1 mg / kg /注射静脉(i.v.)可卡因或接受糖果;然后给4只猴子肌肉注射疫苗,另外2只猴子肌肉注射载体,在整个研究过程中加强疫苗接种。可卡因的增强作用是在自我给药,灭绝和重新获得(复发)阶段进行测量的。在整个研究过程中,接种猴子的血清抗体滴度仍然很高。 6只猴子中有5只在20周内对可卡因的喜好没有改变。 4只(25%)接种猴子中只有一只显示可卡因选择减少。在盐水消光试验中,所有6只猴子都对可卡因熄灭了。接种疫苗的猴子熄灭反应的时间往往比对照猴子要长(17.5 vs. 7.0疗程)。疫苗接种大大阻碍了可卡因自我管理的获得;对照猴子在6至41个疗程内恢复了可卡因的自我管理,并且有1个接种疫苗的猴子在19个疗程中恢复了可卡因的自我管理。其他三只接种疫苗的猴子甚至在采取多种操作鼓励可卡因重新获得的情况下,也需要在57-94次之间恢复可卡因的自我管理。这些数据表明,dAdGNE疫苗对于实现可卡因戒断作为预防复发策略的一部分的人可能具有治疗潜力。

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