Octavio E Fandiño, Aaron R J Hutton, Chunyang Zhang, Marco T A Abbate, Yara A Naser, Yaocun Li, Alejandro J Paredes, Ryan F Donnelly
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To this purpose, HF-MAPs were prepared using poly(vinyl alcohol) (PVA) and poly(vinyl pyrrolidone) (PVP), using citric acid as the crosslinker. Two different reservoirs, containing PVP and PVA as the main components and poly(ethylene)glycol 400 (PEG400) and glycerol as plasticising agents, were used to deliver all the drugs from the HF-MAPs. Franz cells studies in excised neonatal porcine skin demonstrated that the permeation of DMT, 5-MeO-DMT and MES was better from the PEG400 reservoir, showing a permeation of 60.71 %, 59.61 % and 41.85 % respectively. Pharmacokinetic studies in rats showed that HF-MAP technology as a strategy for microdosing psychedelic compounds was also demonstrated with DMT. AUC<sub>t0-final</sub> for the HF-MAP cohort (7186 ± 1296 ng/mL*h) was significantly greater than the IM cohort (1803 ± 53.25 ng/mL*h) (p = 0.0020), with a relative bioavailability of ∼ 72 %. 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引用次数: 0
摘要
纵观历史,迷幻化合物一直被用于宗教、精神和娱乐目的。大量的研究报告使用致幻剂化合物治疗各种疾病,如酗酒、成瘾、抑郁状态到边缘性精神分裂症、人格障碍以及其他精神障碍。致幻剂微剂量是近年来一种常见的技术,涉及为治疗目的而使用小剂量的致幻剂。本研究研究了水凝胶形成微阵列贴片(rf - maps)通过皮肤递送小剂量N,N-二甲基色胺(DMT), 5-甲氧基N,N-二甲基色胺(5-MeO-DMT)和美斯卡林(MES)的潜力。为此,以柠檬酸为交联剂,以聚乙烯醇(PVA)和聚乙烯基吡咯烷酮(PVP)为原料制备了hf - map。两个不同的储层,以PVP和PVA为主要成分,聚乙二醇400 (PEG400)和甘油为增塑剂,用于输送HF-MAPs中的所有药物。新生儿猪皮肤Franz细胞研究表明,PEG400储层对DMT、5-MeO-DMT和MES的通透性更好,分别为60.71 %、59.61 %和41.85 %。大鼠药代动力学研究表明,在DMT中,HF-MAP技术也被证明是一种微剂量迷幻化合物的策略。AUCt0-final HF-MAP队列(7186 ± 1296 ng / mL * h)明显大于IM队列(1803 ±53.25 ng / mL * h) (p = 0.0020),相对生物利用度的 ∼ 72 %。考虑到它们的药代动力学特征,与IM相比,HF-MAP可以减少DMT给药的频率。
Application of microarray patches for the transdermal administration of psychedelic drugs in micro-doses.
Throughout history, psychedelic compounds have been used for religious, spiritual and recreational purposes. A plethora of studies have reported the use of psychedelic compounds in the treatment of various conditions, such as alcoholism, addictions, depressive state to borderline schizophrenia, personality disorder, among other mental disorders. Psychedelic microdosing, a common technique in recent years, involves the consumption of small doses of psychedelic drugs for therapeutic purposes. This study investigated the potential of hydrogel-forming microarray patches (HF-MAPs) to deliver N,N-dimethyltryptamine (DMT), 5-methoxy-N,N-dimethyltryptamine (5-MeO-DMT), and mescaline (MES) in small doses through the skin. To this purpose, HF-MAPs were prepared using poly(vinyl alcohol) (PVA) and poly(vinyl pyrrolidone) (PVP), using citric acid as the crosslinker. Two different reservoirs, containing PVP and PVA as the main components and poly(ethylene)glycol 400 (PEG400) and glycerol as plasticising agents, were used to deliver all the drugs from the HF-MAPs. Franz cells studies in excised neonatal porcine skin demonstrated that the permeation of DMT, 5-MeO-DMT and MES was better from the PEG400 reservoir, showing a permeation of 60.71 %, 59.61 % and 41.85 % respectively. Pharmacokinetic studies in rats showed that HF-MAP technology as a strategy for microdosing psychedelic compounds was also demonstrated with DMT. AUCt0-final for the HF-MAP cohort (7186 ± 1296 ng/mL*h) was significantly greater than the IM cohort (1803 ± 53.25 ng/mL*h) (p = 0.0020), with a relative bioavailability of ∼ 72 %. Considering their pharmacokinetic profile, the frequency of DMT dosing could be reduced with HF-MAP when compared to the IM route.
期刊介绍:
The European Journal of Pharmaceutics and Biopharmaceutics provides a medium for the publication of novel, innovative and hypothesis-driven research from the areas of Pharmaceutics and Biopharmaceutics.
Topics covered include for example:
Design and development of drug delivery systems for pharmaceuticals and biopharmaceuticals (small molecules, proteins, nucleic acids)
Aspects of manufacturing process design
Biomedical aspects of drug product design
Strategies and formulations for controlled drug transport across biological barriers
Physicochemical aspects of drug product development
Novel excipients for drug product design
Drug delivery and controlled release systems for systemic and local applications
Nanomaterials for therapeutic and diagnostic purposes
Advanced therapy medicinal products
Medical devices supporting a distinct pharmacological effect.