Evaluating the Role of Nicotine Stereoisomer on Nicotine Pouch Abuse Liability: A Randomized Crossover Trial.

IF 3 2区医学 Q2 PUBLIC, ENVIRONMENTAL & OCCUPATIONAL HEALTH

Nicotine & Tobacco Research Pub Date : 2025-03-24 DOI:10.1093/ntr/ntae079

Brittney Keller-Hamilton, Hayley Curran, Mahmood Alalwan, Alice Hinton, Marielle C Brinkman, Ahmad El-Hellani, Theodore L Wagener, Kirsten Chrzan, Leanne Atkinson, Sriya Suraapaneni, Darren Mays

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引用次数: 0

Abstract

Introduction: Many oral nicotine pouch (ONP) brands use synthetic nicotine, which typically contains a racemic (50:50) mixture of nicotine's two stereoisomers: S-nicotine and R-nicotine. Because tobacco-derived nicotine contains more than 99% S-nicotine, the effects of R-nicotine in humans are not well known. We compared systemic nicotine exposure and product appeal of ONPs containing more than 99% S-nicotine versus racemic nicotine.

Aims and methods: N = 18 adult smokers (Mage = 45 years, 66.7% male, 77.8% White) enrolled in a three-visit single-blind, randomized crossover study. During each visit, participants used one wintergreen-flavored, 3 mg nicotine ONP for 30 min following at least12 h nicotine abstinence. Study ONP #1 contained more than 99% S-nicotine and the other two study ONPs contained racemic nicotine (collapsed for analyses). Plasma nicotine assessments and measures of withdrawal relief occurred at t = 0, 5, 15, 30, 60, and 90 min; measures of product appeal were assessed following ONP use.

Results: Using the ONP with more than 99% S-nicotine resulted in greater plasma nicotine concentration from 15 to 90 min (p < .0001) and greater maximum plasma nicotine concentration than the ONPs with racemic nicotine (M = 9.9 ng/mL [SD = 2.5] vs. M = 5.7 ng/mL [SD = 2.8], respectively; p < .0001). Product liking and withdrawal relief were similar across ONPs, although participants reported more "bad effects" when using the ONP with more than 99% S-nicotine.

Conclusions: Participants reported few subjective differences in ONPs according to nicotine stereoisomer, but plasma nicotine concentration was greater for ONPs using more than 99% S-nicotine. ONPs with more than 99% S-nicotine (vs. racemic nicotine) might be better substitutes for cigarettes, but research into other ONP characteristics (eg flavors, freebase nicotine) is needed to inform regulation.

Implications: Little is known about the effects of racemic (vs. S-) nicotine in humans. In a sample of adults who smoke cigarettes, we identified that oral nicotine pouches containing racemic nicotine exposed participants to less nicotine than oral nicotine pouches containing only S-nicotine, but both types of oral nicotine pouches held similar, moderate appeal. Additional research evaluating the roles that flavorings, total nicotine concentration, and freebase nicotine play in the abuse liability of oral nicotine pouches would inform comprehensive product regulations to support public health.

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评估尼古丁立体异构体对尼古丁袋滥用可能性的作用：随机交叉试验。

简介：许多口服尼古丁袋（ONP）品牌使用合成尼古丁，其中通常含有尼古丁两种立体异构体的外消旋（50:50）混合物：S-尼古丁和R-尼古丁。由于从烟草中提取的尼古丁含有 99% 以上的 S-尼古丁，因此 R-尼古丁对人体的影响尚不清楚。我们比较了含有 99% 以上 S-尼古丁的 ONPs 与外消旋尼古丁的全身尼古丁暴露量和产品吸引力：N = 18 名成年吸烟者（年龄 = 45 岁，66.7% 为男性，77.8% 为白人）参加了一项为期三次的单盲随机交叉研究。在每次访问期间，参与者在戒断尼古丁至少 12 小时后使用一种冬青味的 3 毫克尼古丁 ONP 30 分钟。1 号研究 ONP 含有 99% 以上的 S-尼古丁，另外两种研究 ONP 含有外消旋尼古丁（分析时折叠）。在 t = 0、5、15、30、60 和 90 分钟时进行血浆尼古丁评估和戒断缓解测量；在使用 ONP 后进行产品吸引力测量：结果：使用 S-尼古丁含量超过 99% 的 ONP 会导致 15 至 90 分钟内血浆尼古丁浓度升高（p 结论：使用 S-尼古丁含量超过 99% 的 ONP 会导致 15 至 90 分钟内血浆尼古丁浓度升高（p）：根据尼古丁立体异构体的不同，受试者对ONP的主观感受差异不大，但使用99%以上S-尼古丁的ONP的血浆尼古丁浓度更高。含有 99% 以上 S-尼古丁的 ONP（与外消旋尼古丁相比）可能是更好的香烟替代品，但还需要对 ONP 的其他特征（如口味、游离基尼古丁）进行研究，以便为监管提供信息：人们对外消旋（与 S-）尼古丁对人体的影响知之甚少。在一个吸食香烟的成年人样本中，我们发现含有外消旋尼古丁的尼古丁口服袋比只含有S-尼古丁的尼古丁口服袋让参与者接触到的尼古丁更少，但两种类型的尼古丁口服袋都具有类似的、适度的吸引力。对香料、尼古丁总浓度和游离基尼古丁在口含尼古丁小袋滥用责任中的作用进行评估的其他研究将为支持公共健康的全面产品法规提供信息。

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来源期刊

Nicotine & Tobacco Research 医学-公共卫生、环境卫生与职业卫生

CiteScore

8.10

自引率

10.60%

发文量

268

审稿时长

3-8 weeks

期刊介绍： Nicotine & Tobacco Research is one of the world''s few peer-reviewed journals devoted exclusively to the study of nicotine and tobacco. It aims to provide a forum for empirical findings, critical reviews, and conceptual papers on the many aspects of nicotine and tobacco, including research from the biobehavioral, neurobiological, molecular biologic, epidemiological, prevention, and treatment arenas. Along with manuscripts from each of the areas mentioned above, the editors encourage submissions that are integrative in nature and that cross traditional disciplinary boundaries. The journal is sponsored by the Society for Research on Nicotine and Tobacco (SRNT). It publishes twelve times a year.