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Larval Zebrafish Model for FDA-Approved Drug Repositioning for Tobacco Dependence Treatment

机译:FDA批准的用于烟草依赖治疗的药物重新定位的幼虫斑马鱼模型

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摘要

Cigarette smoking remains the most preventable cause of death and excess health care costs in the United States, and is a leading cause of death among alcoholics. Long-term tobacco abstinence rates are low, and pharmacotherapeutic options are limited. Repositioning medications approved by the U.S. Food and Drug Administration (FDA) may efficiently provide clinicians with new treatment options. We developed a drug-repositioning paradigm using larval zebrafish locomotion and established predictive clinical validity using FDA-approved smoking cessation therapeutics. We evaluated 39 physician-vetted medications for nicotine-induced locomotor activation blockade. We further evaluated candidate medications for altered ethanol response, as well as in combination with varenicline for nicotine-response attenuation. Six medications specifically inhibited the nicotine response. Among this set, apomorphine and topiramate blocked both nicotine and ethanol responses. Both positively interact with varenicline in the Bliss Independence test, indicating potential synergistic interactions suggesting these are candidates for translation into Phase II clinical trials for smoking cessation.
机译:在美国,抽烟仍然是最可预防的死亡原因和额外的医疗费用,并且是酗酒者中最主要的死亡原因。长期戒烟率低,药物治疗选择有限。重新定位由美国食品药品监督管理局(FDA)批准的药物可能会有效地为临床医生提供新的治疗选择。我们开发了使用幼虫斑马鱼运动的药物替代范例,并使用FDA批准的戒烟疗法建立了可预测的临床有效性。我们评估了39种医师审核的药物对尼古丁引起的运动激活阻滞的影响。我们进一步评估了改变乙醇反应的候选药物,以及与伐尼克兰联合使用对尼古丁反应减弱的作用。六种药物特异性抑制尼古丁反应。在这组药物中,阿扑吗啡和托吡酯阻断了尼古丁和乙醇的反应。两者在Bliss独立性测试中均与伐尼克兰具有积极的相互作用,表明潜在的协同相互作用表明这是翻译成戒烟的II期临床试验的候选者。

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