一种药用大麻制剂在长期高剂量使用阿片类镇痛药的慢性非癌性疼痛患者中的药代动力学、安全性和耐受性:一项试点研究。
Pharmacokinetics, Safety, and Tolerability of a Medicinal Cannabis Formulation in Patients with Chronic Non-cancer Pain on Long-Term High Dose Opioid Analgesia: A Pilot Study.
作者信息
Bonomo Yvonne, Norman Amanda, Collins Lisa, O'Neill Helen, Galettis Peter, Trinca Jane, Strauss Nigel, Martin Jennifer, Castle David
机构信息
Department of Addiction Medicine, St Vincent's Hospital Melbourne, University of Melbourne, P.O. Box 2900, Fitzroy, VIC, 3065, Australia.
Department of Addiction Medicine, St Vincent's Hospital Melbourne, P.O. Box 2900, Fitzroy, VIC, 3065, Australia.
出版信息
Pain Ther. 2022 Mar;11(1):171-189. doi: 10.1007/s40122-021-00344-y. Epub 2021 Dec 18.
INTRODUCTION
This phase I open-label study examined pharmacokinetics, safety, and tolerability of escalating doses of a novel combination cannabinoid medication (1:1 tetrahydrocannabinol [THC]/cannabidiol [CBD]) in patients with chronic non-cancer pain (CNCP) on high dose opioid analgesia.
METHODS
Nine people with CNCP and oral morphine equivalent daily dose of 60 mg or higher were recruited. Blood concentrations of THC, 11-hydroxytetrahydrocannabinol (OH-THC), 11-nor-9-carboxy-tetrahydrocannabinol (COOH-THC), and CBD were assayed weekly. Concentrations were measured after a single dose of 2.5 mg THC/2.5 mg CBD on day 1, and daily escalating doses up to a single dose of 12.5 mg THC/12.5 mg CBD on day 29. Follow-up was on day 36 after a 7-day washout. Secondary outcome data encompassed pain, mood, and sleep parameters.
RESULTS
The parent compounds THC, and CBD, and metabolites OH-THC and COOH-THC were detected at most time points. In general, the concentration of all analytes increased until 2 h post-administration, decreasing to approximately pre-dose concentrations by 8 h. There was considerable inter- and intra-individual variability. The study medication was well tolerated. Eight participants reported at least one adverse event (AE), with a total of 62 AEs; most common were euphoric mood, headache, and agitation, none classified as severe. There was no significant change to pain severity self-ratings, nor use of pain medications. Improvements in pain interference scores, mood, and some sleep parameters were observed.
CONCLUSION
The THC/CBD formulation was tolerated well in a group of patients with CNCP. Between-participant variability supports personalized dosing and "start low-go slow" titration. To validate and quantify improvements in secondary efficacy outcomes a randomized placebo-controlled study is needed.
TRIAL REGISTRATION
Australian New Zealand Clinical Trials Register (CT-2019-CTN-01224-1).
引言
这项I期开放标签研究考察了新型大麻素复方药物(四氢大麻酚[THC]/大麻二酚[CBD]比例为1:1)剂量递增时的药代动力学、安全性及耐受性,研究对象为正在接受高剂量阿片类镇痛药物治疗的慢性非癌性疼痛(CNCP)患者。
方法
招募了9名CNCP患者,其口服吗啡等效日剂量为60毫克或更高。每周检测血液中THC、11-羟基四氢大麻酚(OH-THC)、11-去甲-9-羧基四氢大麻酚(COOH-THC)和CBD的浓度。第1天单次服用2.5毫克THC/2.5毫克CBD后测量浓度,至第29天每日递增剂量直至单次服用12.5毫克THC/12.5毫克CBD。在为期7天的洗脱期后的第36天进行随访。次要结局数据包括疼痛、情绪和睡眠参数。
结果
在大多数时间点均检测到母体化合物THC和CBD以及代谢物OH-THC和COOH-THC。总体而言,所有分析物的浓度在给药后2小时内升高,到8小时时降至接近给药前的浓度。个体间和个体内存在相当大的变异性。研究药物耐受性良好。8名参与者报告了至少1次不良事件(AE),共发生62次AE;最常见的是欣快感、头痛和激动,均无严重不良事件。疼痛严重程度的自我评分及止痛药物的使用情况均无显著变化。观察到疼痛干扰评分、情绪和一些睡眠参数有所改善。
结论
THC/CBD制剂在一组CNCP患者中耐受性良好。参与者之间的变异性支持个性化给药及“低起始、慢增量”滴定。为验证和量化次要疗效结局的改善情况,需要进行一项随机安慰剂对照研究。
试验注册
澳大利亚新西兰临床试验注册中心(CT-2019-CTN-01224-1)
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