健康成年人多次口服两种含Δ9-四氢大麻酚大麻产品的安全性和主观效果的性别差异。

IF 3.1 4区 医学 Q2 PHARMACOLOGY & PHARMACY
Cannabis and Cannabinoid Research Pub Date : 2024-08-01 Epub Date: 2023-08-11 DOI:10.1089/can.2022.0340
Laura MacNair, Graham M L Eglit, Irina Mosesova, Marcel O Bonn-Miller, Erica N Peters
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引用次数: 0

摘要

导言:越来越多的女性表示在使用大麻产品。关于反复口服不同剂量的Δ9-四氢大麻酚(THC,大麻的主要精神活性成分)后的安全性和主观效果的性别差异,目前还缺乏相关数据。材料和方法:数据来自对两种含四氢大麻酚的口服大麻产品进行的两项随机、双盲、安慰剂对照、多剂量、受试者间试验。健康成年人分别服用安慰剂、低剂量四氢大麻酚(每次剂量 2.5 或 5 毫克)或高剂量四氢大麻酚(每次剂量 7.5 或 10 毫克),每天两次,连续服用 7 天。其中男性 38 人(安慰剂 8 人、低剂量 THC 17 人、高剂量 THC 13 人),女性 46 人(安慰剂 8 人、低剂量 THC 17 人、高剂量 THC 21 人)。分析比较了不同 THC 剂量下男性和女性的不良事件(AEs)和主观影响。结果显示在安慰剂组和低剂量 THC 组,AEs 的相对发生率没有性别差异。在高剂量 THC 组中,女性报告的 AEs 是男性的 3.08 倍(95% 置信区间 [CI]=1.31-8.33 倍)。性别×低剂量 THC 组在任何主观效应上都没有明显的交互作用。在高剂量 THC 组,女性对男性的 "放松 "评价更高(b=15.14,95% CI=1.44-28.84,p=0.027),而在安慰剂组,男性对女性的 "喜欢效果 "评价更高(b=-30.01,95% CI=2.77-57.26,p=0.028)。虽然分析不足以评估性别×THC 剂量×天数的交互作用,但高剂量 THC 组在 AEs 和一些主观效应方面的初始性别差异似乎在第一天后缩小了。结论在这项探索性分析中,口服 THC 的某些反应存在细微的性别差异。女性似乎比男性对高剂量而非低剂量的 AEs 和某些主观效应更敏感。在对安慰剂的反应中,男性对某些主观效应的评分高于女性。对高剂量口服 THC 反应的最初性别差异在用药 7 天后趋于减小。如果研究结果得到证实,将有助于为医用大麻产品针对不同性别的剂量策略提供依据,并有助于向医用大麻患者宣传任何时间性效应。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Sex Differences in the Safety and Subjective Effects of Two Oral Δ9-Tetrahydrocannabinol-Containing Cannabis Products over Multiple Doses Among Healthy Adults.

Introduction: A growing number of females report consuming cannabis products. There is a paucity of data on sex differences in safety and subjective effects after repeated use of varying oral doses of Δ9-tetrahydrocannabinol (THC; the primary psychoactive constituent of cannabis). Materials and Methods: Data were from two randomized, double-blind, placebo-controlled, multiple-dose, between-subject trials of two THC-containing oral cannabis products. Healthy adults received placebo, low-dose THC (∼2.5 or ∼5 mg per dose), or high-dose THC (∼7.5 or ∼10 mg per dose) twice daily for 7 days. There were 38 males (8 placebo, 17 low-dose THC, 13 high-dose THC) and 46 females (8 placebo, 17 low-dose THC, 21 high-dose THC). Analyses compared adverse events (AEs) and subjective effects between males and females, by THC dose. Results: In the placebo and low-dose THC groups, there were no sex differences in the relative rate of AEs. In the high-dose THC group, females versus males reported 3.08 (95% confidence interval [CI]=1.31-8.33) times as many AEs. There were no significant interactions of sex×low-dose THC group for any subjective effect. In the high-dose THC group, females versus males reported greater "relaxed" ratings (b=15.14, 95% CI=1.44-28.84, p=0.027), whereas in the placebo group, males versus females reported greater ratings of "liking the effect" (b=-30.01, 95% CI=2.77-57.26, p=0.028). Although analyses were underpowered to assess the sex×THC dose×day interaction, the initial sex disparity in AEs and some subjective effects in the high-dose THC group appeared to shrink after the first day. Conclusions: In this exploratory analysis, sex differences in some responses to oral THC were nuanced. Females appeared more sensitive than males to AEs and some subjective effects at higher but not lower doses. Males reported higher ratings than females on some subjective effects in response to placebo. Initial sex differences in response to higher doses of oral THC tended to diminish over 7 days of dosing. If replicated, findings could help inform sex-specific dosing strategies of medical cannabis products and could help educate medical cannabis patients on any temporality of effects.

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来源期刊
Cannabis and Cannabinoid Research
Cannabis and Cannabinoid Research PHARMACOLOGY & PHARMACY-
CiteScore
6.80
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7.90%
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164
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