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麻黄碱、黄嘌呤和前列腺素抑制剂:产热刺激中的作用及相互作用

Ephedrine, xanthines and prostaglandin-inhibitors: actions and interactions in the stimulation of thermogenesis.

作者信息

Dulloo A G

机构信息

Department of Physiology, Centre Médical Universitaire, Geneva, Switzerland.

出版信息

Int J Obes Relat Metab Disord. 1993 Feb;17 Suppl 1:S35-40.

PMID:8384178
Abstract

The pivotal role of the sympathoadrenal system in the defense of le milieu interieur has, in the last 15 years, been extended to include the fat stores-a notion that forms the basis of current strategies for thermogenic stimulation in obesity therapy. The search for effective and safe sympathetic stimulants has been directed at two main levels: (i) the development of novel beta-agonists selective for thermogenesis, and (ii) the evaluation of drugs already in clinical use for other purposes (e.g. ephedrine) which could conceivably increase the release of catecholamines to levels that enhance thermogenesis without significant cardiovascular effects. A re-direction of these strategies seem inevitable because at therapeutic doses, the thermogenic effects of these sympathomimetics seem to be considerably dampened by negative feedback mechanisms that operate both extracellularly (e.g. via adenosine & prostaglandins) as well as inside the cells (via cAMP phosphodiesterases). Such a contention is supported by studies both in man and in animals showing that methylxanthines and aspirin, drugs known to be capable of interfering with these modulators, potentiate the thermogenic effects of ephedrine. Future research aimed at clarifying the types and subtypes of these negative modulators of sympathomimetic-induced thermogenesis and their targeting by more selective antagonists would no doubt be pivotal in providing the safe drug combination with the necessary thermogenic properties to assist the management of obesity.

摘要

在过去15年里,交感肾上腺系统在维持内环境稳定中的关键作用已扩展至包括脂肪储备——这一概念构成了当前肥胖治疗中热生成刺激策略的基础。对有效且安全的交感神经兴奋剂的探索主要集中在两个层面:(i)开发对产热有选择性的新型β-激动剂,以及(ii)评估已用于其他目的的临床药物(如麻黄碱),这些药物可能会将儿茶酚胺释放量提高到能增强产热而无明显心血管效应的水平。这些策略的重新调整似乎不可避免,因为在治疗剂量下,这些拟交感神经药的产热效应似乎会被细胞外(如通过腺苷和前列腺素)以及细胞内(通过环磷酸腺苷磷酸二酯酶)起作用的负反馈机制显著抑制。人体和动物研究均支持这一观点,这些研究表明,已知能够干扰这些调节剂的甲基黄嘌呤和阿司匹林可增强麻黄碱的产热效应。未来旨在阐明拟交感神经药诱导产热的这些负调节剂的类型和亚型,以及通过更具选择性的拮抗剂对其进行靶向作用的研究,无疑将为提供具有必要产热特性的安全药物组合以辅助肥胖管理起到关键作用。

相似文献

1
Ephedrine, xanthines and prostaglandin-inhibitors: actions and interactions in the stimulation of thermogenesis.麻黄碱、黄嘌呤和前列腺素抑制剂:产热刺激中的作用及相互作用
Int J Obes Relat Metab Disord. 1993 Feb;17 Suppl 1:S35-40.
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Thermogenesis in human brown adipose tissue and skeletal muscle induced by sympathomimetic stimulation.拟交感神经刺激诱导的人体棕色脂肪组织和骨骼肌产热。
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Peripheral mechanisms of thermogenesis induced by ephedrine and caffeine in brown adipose tissue.
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The thermogenic properties of ephedrine/methylxanthine mixtures: human studies.麻黄碱/甲基黄嘌呤混合物的产热特性:人体研究。
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Potentiation of the thermogenic antiobesity effects of ephedrine by dietary methylxanthines: adenosine antagonism or phosphodiesterase inhibition?膳食甲基黄嘌呤对麻黄碱产热抗肥胖作用的增强:腺苷拮抗还是磷酸二酯酶抑制?
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