Nicotine flux and pharmacokinetics-based considerations for early assessment of nicotine delivery systems

Aditya R. Kolli , Emilija Veljkovic , Florian Calvino-Martin , Marco Esposito , Arkadiusz K. Kuczaj , Ondrej Koumal , Jed E. Rose , Manuel C. Peitsch
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Abstract

In the past few years, technological advancements enabled the development of novel electronic nicotine delivery systems (ENDS). Several empirical measures such as “nicotine flux” are being proposed to evaluate the abuse liability potential of these products. We explored the applicability of nicotine flux for clinical nicotine pharmacokinetics (PK) and 52-week quit success from cigarettes for a wide range of existing nicotine delivery systems. We found that the differences in nicotine flux for various nicotine delivery systems are not related to changes in PK, as nicotine flux does not capture key physiological properties such as nicotine absorption rate. Further, the 52-week quit success and abuse liability potential of nicotine nasal sprays (high nicotine flux product), and nicotine inhalers (nicotine flux similar to ENDS) are low, suggesting that nicotine flux is a poor metric for the assessment of nicotine delivery systems. PK indices are more dependable for characterizing nicotine delivery systems, and a nicotine plasma CmaxTmax > 1 could improve 52-week quit success from cigarettes. However, a single metric may be inadequate to fully assess the abuse liability potential of nicotine delivery systems and needs to be further studied. A combination of in vitro and in silico approaches could potentially address the factors influencing the inhaled aerosol dosimetry and resulting PK of nicotine to provide early insights for ENDS assessments. Further research is required to understand nicotine dosimetry and PK for ad libitum product use, and abuse liability indicators of nicotine delivery systems. This commentary is intended to (1) highlight the need to think beyond a single empirical metric such as nicotine flux, (2) suggest potential PK-based metrics, (3) suggest the use of in vitro and in silico tools to obtain early insights into inhaled aerosol dosimetry for ENDS, and (4) emphasize the importance of considering comprehensive clinical pharmacology outcomes to evaluate nicotine delivery systems.

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尼古丁输送系统早期评估中基于尼古丁通量和药代动力学的考虑因素
过去几年中,技术进步推动了新型电子尼古丁输送系统(ENDS)的发展。人们提出了 "尼古丁通量 "等几种经验性指标来评估这些产品的滥用可能性。我们探讨了尼古丁通量对现有各种尼古丁给药系统的临床尼古丁药代动力学(PK)和 52 周戒烟成功率的适用性。我们发现,不同尼古丁给药系统的尼古丁通量差异与药代动力学变化无关,因为尼古丁通量不能反映尼古丁吸收率等关键生理特性。此外,尼古丁鼻腔喷雾剂(尼古丁通量高的产品)和尼古丁吸入器(尼古丁通量与ENDS相似)的52周戒烟成功率和滥用可能性都很低,这表明尼古丁通量是评估尼古丁给药系统的一个较差指标。PK指数对于描述尼古丁给药系统的特征更为可靠,尼古丁血浆CmaxTmax > 1可提高52周戒烟成功率。然而,单一指标可能不足以全面评估尼古丁给药系统的滥用潜力,因此需要进一步研究。将体外和硅学方法结合起来,有可能解决影响尼古丁吸入气溶胶剂量测定和由此产生的PK的因素,从而为ENDS评估提供早期见解。需要进一步开展研究,以了解自由使用产品时的尼古丁剂量测定和PK,以及尼古丁给药系统的滥用责任指标。本评论旨在:(1) 强调超越尼古丁通量等单一经验指标的必要性;(2) 建议潜在的基于PK的指标;(3) 建议使用体外和硅学工具及早了解ENDS的吸入气溶胶剂量学;(4) 强调在评估尼古丁给药系统时考虑综合临床药理结果的重要性。
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Drug and alcohol dependence reports
Drug and alcohol dependence reports Psychiatry and Mental Health
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