Artificial Sweeteners in US-Marketed Oral Nicotine Pouch Products: Correlation with Nicotine Contents and Effects on Product Preference.

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

Nicotine & Tobacco Research Pub Date : 2024-12-05 DOI:10.1093/ntr/ntae293

Sairam V Jabba, Peter Silinski, Alicia Y Yang, Wenyi Ouyang, Sven E Jordt

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引用次数: 0

Abstract

Introduction: Artificial sweeteners, sucralose and acesulfame-k, are listed as ingredients of oral nicotine pouches (ONPs), a product category with rapidly growing market share. The exact quantities of these sweeteners in ONPs remain unknown. Artificial sweeteners in ONPs may reduce aversion, facilitate initiation and encourage consumption behavior.

Methods: Sucralose and acesulfame-k contents in major US-marketed ONP brands (Zyn, on!, Velo) were determined by Liquid-Chromatography-Mass-Spectrometry. Sweetener effects on aversion and consumption of ONP's were modeled in single- and two-bottle drinking tests, offering mice ONP extracts calibrated to contain nicotine levels similar to saliva of people who use smokeless tobacco. To examine the contribution of sweet taste perception, consumption behavior was compared between wild-type and sweet-taste receptor deficient mice (Tas1r2-/-).

Results: Acesulfame-K was detected in on!, Zyn and Velo ONPs (~0.3 to 0.9mg/pouch), including products marketed as "Unflavored" or "Flavor ban approved". In Velo ONPs, sweetened with sucralose (~0.6 to1.2mg/pouch), higher nicotine strength products contained higher sucralose levels. Tas1r2-/- mice consumed less ONP extracts than wild-type mice in both sexes. ONP extracts with both higher nicotine and sweetener strengths were tolerated by wild-type mice, but produced stronger aversion in Tas1r2-/- mice.

Conclusions: ONPs contain significant amounts of artificial sweeteners acesulfame-k and sucralose, with some brands adding more sweetener to higher nicotine strength ONPs. In mice, artificial sweeteners, at levels present in ONPs, increase nicotine consumption. Increasing sweetener contents facilitate consumption of higher nicotine strength ONPs. Sweetness imparted by sweetener addition to ONPs likely reduces aversive sensory effects of nicotine and other ONP constituents.

Implications: Artificial sweeteners such as acesulfame-K or sucralose reduce aversion and likely facilitate consumption of ONPs. The marketing of some artificially sweetened ONPs as "Unflavored" or "Flavor ban-approved" suggests that the tobacco industry rejects sweet taste as a determinant for the presence of a characterizing flavor. Sweetness as imparted by artificial sweeteners in tobacco products needs to be addressed by regulators as a component of a characterizing flavor, with the aim to reduce product appeal and initiation by never users, and especially youth attracted to sweet flavors.

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在美国销售的口服尼古丁袋装产品中的人工甜味剂：与尼古丁含量的相关性和对产品偏好的影响。

导言：人工甜味剂蔗糖素(三氯蔗糖)和安赛蜜(安赛蜜-k)被列为口服尼古丁袋(ONPs)的成分，ONPs是一种市场份额迅速增长的产品类别。这些甜味剂在口服尼古丁袋中的确切含量仍不得而知。口服尼古丁袋中的人工甜味剂可能会降低厌恶感、促进开始吸食和鼓励消费行为：方法：采用液相色谱-质谱法测定了美国市场上主要 ONP 品牌（Zyn、on!在单瓶和双瓶饮用测试中模拟了甜味剂对ONP的厌恶和消费的影响，为小鼠提供了ONP提取物，其尼古丁含量与使用无烟烟草者的唾液含量相似。为了研究甜味感知的贡献，比较了野生型小鼠和甜味受体缺陷小鼠（Tas1r2-/-）的消费行为：结果：在on！、Zyn和Velo ONPs（~0.3至0.9毫克/袋）中检测到了安赛蜜-K，包括市场上标注为 "无味 "或 "禁味 "的产品。在用蔗糖素(三氯蔗糖)增甜的Velo ONPs（约0.6至1.2毫克/袋）中，尼古丁浓度较高的产品含有较高的蔗糖素(三氯蔗糖)含量。与野生型小鼠相比，Tas1r2-/-小鼠（雌雄均有）摄入的 ONP 提取物较少。野生型小鼠可以耐受尼古丁和甜味剂强度较高的ONP提取物，但Tas1r2-/-小鼠会产生更强的厌恶感：结论：ONP含有大量人工甜味剂安赛蜜和三氯蔗糖，一些品牌在尼古丁浓度较高的ONP中添加了更多甜味剂。在小鼠体内，人造甜味剂在 ONP 中的含量会增加尼古丁的消耗量。增加甜味剂含量有助于消费尼古丁浓度较高的烟片。甜味剂添加到ONP中带来的甜味可能会降低尼古丁和其他ONP成分的厌恶感觉效应：影响：安赛蜜-K 或蔗糖素(三氯蔗糖)等人工甜味剂可降低厌恶感，并可能促进吸食 ONP。一些人工甜味 ONP 在市场上标榜 "无味 "或 "禁用香精"，这表明烟草行业拒绝将甜味作为是否存在特征性香味的决定因素。烟草制品中的人工甜味剂所带来的甜味需要由监管机构作为特征风味的一个组成部分来处理，目的是减少产品的吸引力和从未吸食者，特别是被甜味所吸引的年轻人的初次吸食。

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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.