厌食症:对恒河猴食物摄入和自我管理的影响。

Alcohol and drug research Pub Date : 1987-01-01
R L Corwin, W L Woolverton, C R Schuster, C E Johanson
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引用次数: 0

摘要

研究人员将厌食症药物苯非他明、氯芬特明、氯特明、马辛多尔、苯地美拉津和苯美拉津对食物摄入的影响与d-安非他明对恒河猴每天摄入食物颗粒的影响进行了比较。在恒河猴中也确定了这些化合物在固定比例10时间表下维持静脉自我给药的能力。所有药物都以剂量相关的方式减少食物摄入量。d-安非他明是最有效的。马茚多、氯芬特明、苯甲曲明和苯甲曲明的效力约为d-安非他明的1/5至1/9,苯丙他明和氯定的效力分别为d-安非他明的1/14和1/20。苯丙胺、马辛多尔和苯美曲嗪在生理盐水水平以上自行给药,其效力大致相等。氯芬特明和氯替宁不能自行给药,而苯地美嗪只能由四只猴子中的一只自行给药。因此,尽管所有化合物都是有效的厌食药,但氯芬特明、氯替特和苯地美嗪并没有作为正强化剂的作用。由于药物作为正强化物的能力与其依赖性有关,这三种化合物在治疗时可能较少被滥用。在三种自我给药的化合物中,苯丙胺作为一种正强化剂比作为一种厌食症药相对更有效。因此,对于治疗用途,这种药物可能是一种不太理想的化合物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Anorectics: effects on food intake and self-administration in rhesus monkeys.

The effects of the anorectics benzphetamine, chlorphentermine, clortermine, mazindol, phendimetrazine, and phenmetrazine on food intake were compared to the effects of d-amphetamine in rhesus monkeys given daily access to food pellets. The ability of these compounds to maintain intravenous self-administration under a fixed-ratio 10 schedule was also determined in rhesus monkeys. All drugs reduced food intake in a dose-related manner. d-Amphetamine was the most potent. Mazindol, chlorphentermine, phenmetrazine, and phendimetrazine were approximately 1/5 to 1/9 as potent as d-amphetamine while benzphetamine and clortermine were 1/14 and 1/20 as potent, respectively. Benzphetamine, mazindol, and phenmetrazine were self-administered above saline levels and were approximately equipotent. Chlorphentermine and clortermine were not self-administered and phendimetrazine was self-administered by only one of four monkeys at one dose. Thus, although all of the compounds were effective anorectics, chlorphentermine, clortermine, and phendimetrazine did not function as positive reinforcers. Since the ability of a drug to function as a positive reinforcer is related to its dependence potential, these three compounds might be less subject to abuse when used therapeutically. Within the group of 3 compounds that was self-administered, benzphetamine was relatively more potent as a positive reinforcer than as an anorectic. Therefore, this drug might be a less desirable compound for therapeutic use.

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