新型丁丙诺啡/纳洛酮舌下片用于阿片类药物替代治疗的药代动力学和药物学特性与健康志愿者中常规丁丙诺啡/纳洛酮舌下片的比较。

Pharmacokinetic and pharmaceutical properties of a novel buprenorphine/naloxone sublingual tablet for opioid substitution therapy versus conventional buprenorphine/naloxone sublingual tablet in healthy volunteers.

机构信息

Orexo AB, Rapsgatan 7E, SE-754 50 Uppsala, Sweden.

Mundipharma Research Limited, Cambridge Science Park, Milton Road, Cambridge CB4 0AB, United Kingdom.

出版信息

Eur J Pharm Sci. 2018 Sep 15;122:125-133. doi: 10.1016/j.ejps.2018.06.024. Epub 2018 Jun 22.

DOI:10.1016/j.ejps.2018.06.024

PMID:29940217

Abstract

PURPOSE

A novel sublingual buprenorphine/naloxone rapidly-dissolving tablet (BNX-RDT) for opioid substitution therapy has been developed for improved bioavailability, rapid disintegration and improved taste masking. We compared the bioavailability and pharmaceutical properties of BNX-RDT with conventional buprenorphine/naloxone sublingual tablets (BNX).

METHODS

Fasting, open-label, randomized, single-dose, two-cohort crossover study in healthy volunteers under naltrexone block. Cohort 1 (high-dose, N = 64) received BNX-RDT 11.4/2.9 mg and BNX 16/4 mg. Cohort 2 (low-dose, N = 61) received BNX-RDT 2.9/0.71 mg and BNX 4/1 mg. Plasma samples were collected over 72 h. Relative systemic exposures of buprenorphine and naloxone were assessed using standard statistical models for bioequivalence analysis. Pharmaceutical assessments included dissolve time, taste and mouthfeel assessments, and overall preference.

RESULTS

BNX-RDT 11.4/2.9 mg provided equivalent buprenorphine and naloxone exposure to BNX 16/4 mg. BNX-RDT 2.9/0.71 mg provided ~20% lower buprenorphine and 35% lower naloxone exposure compared with BNX 4/1 mg. The comparison of BNX-RDT 2.9/0.71 mg with BNX 4/1 mg did not fully meet equivalence criteria. BNX-RDT was associated with improved dose proportionality across strengths compared with BNX (post hoc analysis), resulting in lower exposure from BNX-RDT relative to BNX at the lower strength. Median perceived dissolve times were significantly shorter for BNX-RDT than BNX at high (8.5 versus 16.2 min) and low (7.6 versus 9.1 min) doses. Taste and mouthfeel were rated significantly more pleasant than BNX, with ~78% of subjects preferring BNX-RDT.

CONCLUSION

BNX-RDT provided improved buprenorphine absorption compared to a conventional sublingual tablet, with shorter dissolve times and improved taste and mouthfeel, resulting in a high preference for the novel formulation.

摘要

目的

为提高生物利用度、快速崩解和改善味觉掩蔽，开发了一种新型舌下丁丙诺啡/纳洛酮速溶片（BNX-RDT）用于阿片类药物替代治疗。我们比较了 BNX-RDT 与常规舌下丁丙诺啡/纳洛酮片（BNX）的生物利用度和药物特性。

方法

在纳曲酮阻断下，健康志愿者进行禁食、开放标签、随机、单剂量、两队列交叉研究。队列 1（高剂量，N=64）接受 BNX-RDT 11.4/2.9mg 和 BNX 16/4mg。队列 2（低剂量，N=61）接受 BNX-RDT 2.9/0.71mg 和 BNX 4/1mg。采集 72 小时的血浆样本。采用标准生物等效性分析统计模型评估丁丙诺啡和纳洛酮的相对系统暴露。药物评估包括溶解时间、口味和口感评估以及总体偏好。

结果

BNX-RDT 11.4/2.9mg 提供与 BNX 16/4mg 相当的丁丙诺啡和纳洛酮暴露。BNX-RDT 2.9/0.71mg 与 BNX 4/1mg 相比，丁丙诺啡和纳洛酮暴露分别降低约 20%和 35%。BNX-RDT 2.9/0.71mg 与 BNX 4/1mg 的比较未完全符合等效标准。与 BNX 相比，BNX-RDT 在各剂量强度下均具有更好的剂量比例关系（事后分析），因此在较低强度时，BNX-RDT 的暴露量相对低于 BNX。高剂量（8.5 分钟比 16.2 分钟）和低剂量（7.6 分钟比 9.1 分钟）时，BNX-RDT 的中位感知溶解时间明显短于 BNX。味道和口感的评价明显优于 BNX，约 78%的受试者更喜欢 BNX-RDT。