首页> 美国卫生研究院文献>The Journal of Pharmacology and Experimental Therapeutics >Repeated Administration of a Mutant Cocaine Esterase: Effects on Plasma Cocaine Levels Cocaine-Induced Cardiovascular Activity and Immune Responses in Rhesus Monkeys
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Repeated Administration of a Mutant Cocaine Esterase: Effects on Plasma Cocaine Levels Cocaine-Induced Cardiovascular Activity and Immune Responses in Rhesus Monkeys

机译:重复施用突变型可卡因酯酶:对恒河猴血浆可卡因水平可卡因诱导的心血管活性和免疫反应的影响

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摘要

Previous studies have demonstrated the capacity of a long-acting mutant form of a naturally occurring bacterial double mutant cocaine esterase (DM CocE) to antagonize the reinforcing, discriminative, convulsant, and lethal effects of cocaine in rodents and reverse the increases in mean arterial pressure (MAP) and heart rate (HR) produced by cocaine in rhesus monkeys. This study was aimed at characterizing the immunologic responses to repeated dosing with DM CocE and determining whether the development of anti-CocE antibodies altered the capacity of DM CocE to reduce plasma cocaine levels and ameliorate the cardiovascular effects of cocaine in rhesus monkeys. Under control conditions, intravenous administration of cocaine (3 mg/kg) resulted in a rapid increase in the plasma concentration of cocaine (n = 2) and long-lasting increases in MAP and HR (n = 3). Administration of DM CocE (0.32 mg/kg i.v.) 10 min after cocaine resulted in a rapid hydrolysis of cocaine with plasma levels below detection limits within 5 to 8 min. Elevations in MAP and HR were significantly reduced within 25 and 50 min of DM CocE administration, respectively. Although slight (10-fold) increases in anti-CocE antibodies were observed after the fourth administration of DM CocE, these antibodies did not alter the capacity of DM CocE to reduce plasma cocaine levels or ameliorate cocaine's cardiovascular effects. Anti-CocE titers were transient and generally dissipated within 8 weeks. Together, these results suggest that highly efficient cocaine esterases, such as DM CocE, may provide a novel and effective therapeutic for the treatment of acute cocaine intoxication in humans.
机译:先前的研究表明,长效突变体形式的天然细菌双突变体可卡因酯酶(DM CocE)能够拮抗可卡因在啮齿动物中的增强,区分,惊厥和致死作用,并逆转平均动脉压的升高(MAP)和可卡因在恒河猴中产生的心率(HR)。这项研究旨在表征对DM CocE重复给药的免疫反应,并确定抗CocE抗体的开发是否改变了DM CocE降低血浆可卡因水平和改善可卡因在恒河猴中的心血管作用的能力。在对照条件下,静脉注射可卡因(3 mg / kg)可卡因的血浆浓度迅速增加(n = 2),而MAP和HR持久增加(n = 3)。可卡因后10分钟给予DM CocE(0.32 mg / kg静脉内),可卡因迅速水解,血浆水平在5至8分钟内低于检测极限。 DM CocE给药后25分钟和50分钟内,MAP和HR的升高显着降低。尽管在第四次服用DM CocE后观察到抗CocE抗体的轻微增加(10倍),但这些抗体并未改变DM CocE降低血浆可卡因水平或改善可卡因的心血管作用的能力。抗CocE滴度是短暂的,通常在8周内消失。总之,这些结果表明,高效可卡因酯酶,例如DM CocE,可为治疗人类急性可卡因中毒提供新颖有效的治疗方法。

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