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对抗合成大麻素 PB-22 的药代动力学方法。

Pharmacokinetic Approach to Combat the Synthetic Cannabinoid PB-22.

机构信息

Department of Chemistry, Department of Immunology and Microbial Science, The Skaggs Institute for Chemical Biology, and The Worm Institute for Research and Medicine (WIRM), The Scripps Research Institute, 10550 North Torrey Pines Road, La Jolla, California 92037, United States.

出版信息

ACS Chem Neurosci. 2021 Jul 21;12(14):2573-2579. doi: 10.1021/acschemneuro.1c00360. Epub 2021 Jul 13.

Abstract

Synthetic cannabinoids are part of a group of drugs called new psychoactive substances. Most of these cannabinoids are unregulated, and there are no therapeutic treatments for their addictive properties or reversing a potential overdose. Vaccination and catalytic antibodies strategies were investigated to assess their ability to blunt the psychoactive properties of the cannabinoid PB-22. To complement these antibody concentric investigations, we also disclose the discovery of the enzymatic degradation of this cannabinoid. Serum factors including albumin and carboxylesterase were found to catalyze the hydrolysis of PB-22. Affinity, kinetics, animal behavior, and biodistribution studies were utilized to evaluate the efficiency of these pharmacokinetic approaches. Our findings suggest simple antibody binding as the most efficacious means for altering PB-22's effect on the brain. Catalytic approaches only translated to esterases being capable of PB-22's degradation with a catalytic antibody approach providing no proclivity for PB-22's hydrolysis. Pharmacokinetic approaches provide a powerful strategy for treating substance abuse disorders and overdose for drugs where no therapeutic is available.

摘要

合成大麻素是一类被称为新精神活性物质的药物的一部分。这些大麻素大多数都不受管制,也没有针对其成瘾性或逆转潜在过量的治疗方法。本研究调查了疫苗接种和催化抗体策略,以评估它们减轻大麻素 PB-22 致幻特性的能力。为了补充这些抗体同心研究,我们还披露了发现这种大麻素的酶促降解。发现血清因子包括白蛋白和羧酸酯酶可催化 PB-22 的水解。利用亲和性、动力学、动物行为和生物分布研究来评估这些药代动力学方法的效率。我们的研究结果表明,简单的抗体结合是改变 PB-22 对大脑影响的最有效方法。催化方法仅表明酯酶能够降解 PB-22,而催化抗体方法对 PB-22 的水解没有倾向性。药代动力学方法为治疗物质滥用障碍和没有治疗方法的药物过量提供了一种强有力的策略。

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