半合成四环素衍生物对高乙醇饮用的有效还原。

IF 3.2 3区 医学 Q1 Medicine
P. Syapin, Joseph M. Martinez, D. Curtis, P. Marquardt, C. L. Allison, J. A. Groot, Carol Baby, Yazan M. Al-Hasan, Ismael Segura, Matthew J Scheible, Katy T Nicholson, J. Redondo, David R. M. Trotter, David S. Edwards, S. Bergeson
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引用次数: 16

摘要

背景:需要新的药物疗法来治疗酒精使用障碍(AUD)。鉴于AUD的复杂性,可能存在多种新的药物靶点。我们和其他人已经证明,四环素类药物,二甲胺四环素和多西环素,减少了小鼠的乙醇(EtOH)饮用。为了验证四环素抑制高EtOH消耗是其普遍特性的假设,我们使用在黑暗中饮酒(DID)范式筛选了几种抗饮酒活性的衍生物。利用剂量-反应关系对活性药物进行进一步研究。方法成年雌性和雄性C57BL/6J小鼠单独饲养,采用20% EtOH,为期4 d。小鼠在饮酒前20小时服用四环素或其载体。每天测量水和EtOH的消耗量。在药物注射开始时和实验最后一天后测量体重。在最后一次饮酒后立即采集血液进行EtOH含量测定。结果7种四环素类药物以50mg /kg剂量检测。只有米诺环素和替加环素显著减少EtOH饮酒,多西环素对减少饮酒表现出较强的效应量趋势。随后对这三种药物的研究表明,雌性和雄性小鼠的EtOH消耗量均呈剂量依赖性下降,但在功效上存在性别差异。二甲胺四环素和多西环素在高剂量下减少了水的摄入量,尽管程度低于它们对EtOH饮酒的影响。替加环素对饮水量没有负面影响。降低EtOH消耗的效价顺序为米诺环素>强力环素>替加环素,说明药效与它们的分配系数和分布常数没有严格的关系。结论替加环素具有降低高EtOH消耗且不影响饮水量的作用,是最有希望开发治疗AUD新药物的四环素类先导化合物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Effective Reduction in High Ethanol Drinking by Semisynthetic Tetracycline Derivatives.
BACKGROUND New pharmacotherapies to treat alcohol use disorders (AUD) are needed. Given the complex nature of AUD, there likely exist multiple novel drug targets. We, and others, have shown that the tetracycline drugs, minocycline and doxycycline, reduced ethanol (EtOH) drinking in mice. To test the hypothesis that suppression of high EtOH consumption is a general property of tetracyclines, we screened several derivatives for antidrinking activity using the Drinking-In-the-Dark (DID) paradigm. Active drugs were studied further using the dose-response relationship. METHODS Adult female and male C57BL/6J mice were singly housed and the DID paradigm was performed using 20% EtOH over a 4-day period. Mice were administered a tetracycline or its vehicle 20 hours prior to drinking. Water and EtOH consumption was measured daily. Body weight was measured at the start of drug injections and after the final day of the experiment. Blood was collected for EtOH content measurement immediately following the final bout of drinking. RESULTS Seven tetracyclines were tested at a 50 mg/kg dose. Only minocycline and tigecycline significantly reduced EtOH drinking, and doxycycline showed a strong effect size trend toward reduced drinking. Subsequent studies with these 3 drugs revealed a dose-dependent decrease in EtOH consumption for both female and male mice, with sex differences in efficacy. Minocycline and doxycycline reduced water intake at higher doses, although to a lesser degree than their effects on EtOH drinking. Tigecycline did not negatively affect water intake. The rank order of potency for reduction in EtOH consumption was minocycline > doxycycline > tigecycline, indicating efficacy was not strictly related to their partition coefficients or distribution constants. CONCLUSIONS Due to its effectiveness in reducing high EtOH consumption coupled without an effect on water intake, tigecycline was found to be the most promising lead tetracycline compound for further study toward the development of a new pharmacotherapy for the treatment of AUD.
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来源期刊
CiteScore
5.90
自引率
9.40%
发文量
219
审稿时长
1 months
期刊介绍: Alcoholism: Clinical and Experimental Research''s scope spans animal and human clinical research, epidemiological, experimental, policy, and historical research relating to any aspect of alcohol abuse, dependence, or alcoholism. This journal uses a multi-disciplinary approach in its scope of alcoholism, its causes, clinical and animal effect, consequences, patterns, treatments and recovery, predictors and prevention.
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