鼻内芬太尼喷雾剂在癌症爆发性疼痛患者中的疗效与耐受性

Efficacy and tolerability of intranasal fentanyl spray in cancer patients with breakthrough pain.

作者信息

Thronæs Morten, Popper Lars, Eeg Martin, Jaatun Ellen, Kvitberg Magnar, Kaasa Stein

机构信息

Norwegian University of Science and Technology, Faculty of Medicine, Department of Cancer Research and Molecular Medicine, European Palliative Care Research Centre, Trondheim, Norway; St Olavs Hospital, Trondheim University Hospital, Cancer Clinic, Trondheim, Norway.

Takeda Pharma A/S, Clinical Science, Roskilde, Denmark.

出版信息

Clin Ther. 2015 Mar 1;37(3):585-96. doi: 10.1016/j.clinthera.2014.12.010. Epub 2015 Jan 30.

DOI:10.1016/j.clinthera.2014.12.010

PMID:25641199

Abstract

PURPOSE

The aims of this study were to explore the efficacy of intranasal fentanyl spray* (INFS) 400 μg to evaluate 12-week tolerability of the nasal mucosa and to explore safety data for all dose strengths of INFS in patients with cancer-related breakthrough pain (BTP).

METHODS

Patients received a test dose of INFS 50 μg, followed by a titration phase. Those patients with doses titrated to 200 or 400 μg entered a randomized, double-blind, cross-over efficacy phase, in which 8 episodes of BTP were randomly treated with INFS 400 μg (6 episodes) and placebo (2 episodes), followed by a tolerability phase. Patients with doses titrated to 50 or 100 μg entered the tolerability phase directly. Primary outcome was measured by pain intensity difference at 10 minutes, analyzed using ANCOVA, and presented as least square mean difference. Examination of the nasal cavity was conducted at inclusion and after 12 weeks of treatment by an otorhinolaryngologist.

FINDINGS

Forty-six patients were included. Thirty-eight patients' doses were titrated to an effective dose of INFS; 50 μg (n = 8), 100 μg (n = 9), 200 μg (n = 9), and 400 μg (n = 12); 15 patients entered the efficacy phase and 31 entered the tolerability phase. In the efficacy phase, 88 and 29 episodes of BTP were treated with INFS 400 μg and placebo, respectively. Pain intensity difference at 10 minutes least square mean for INFS 400 μg was 2.5 (95% CI, 1.42-3.49) (P < 0.001) and least square mean difference between INFS 400 μg and placebo was 1.1 (95% CI, 0.41-1.79) (P = 0.002). Runny nose (10%) and change in color of the mucosa (9%) were the most frequent findings of nasal examination, and nausea and dizziness were the most frequent treatment-related adverse events. One serious adverse event (ie, respiratory depression) was considered related to INFS.

IMPLICATIONS

INFS 400 μg is effective and nasal tolerability and overall safety profile is acceptable during 12 weeks of use. ClinicalTrials.gov identifier: NCT01429051.

摘要

目的

本研究旨在探讨400μg鼻内芬太尼喷雾剂（INFS）的疗效，评估鼻黏膜12周的耐受性，并探索INFS所有剂量强度在癌症相关突破性疼痛（BTP）患者中的安全性数据。

方法

患者接受50μg的INFS试验剂量，随后进入滴定阶段。那些剂量滴定至200或400μg的患者进入随机、双盲、交叉疗效阶段，其中8次BTP发作分别用400μg INFS（6次发作）和安慰剂（2次发作）随机治疗，随后进入耐受性阶段。剂量滴定至50或100μg的患者直接进入耐受性阶段。主要结局通过10分钟时的疼痛强度差异进行测量，采用协方差分析进行分析，并以最小二乘均值差异表示。在纳入时和治疗12周后，由耳鼻喉科医生对鼻腔进行检查。

结果

纳入46例患者。38例患者的剂量滴定至INFS有效剂量；50μg（n = 8）、100μg（n = 9）、200μg（n = 9）和400μg（n = 12）；15例患者进入疗效阶段，31例进入耐受性阶段。在疗效阶段，分别用400μg INFS和安慰剂治疗88次和29次BTP发作。400μg INFS在10分钟时的疼痛强度差异最小二乘均值为2.5（95%CI，1.42 - 3.49）（P < 0.001），400μg INFS与安慰剂之间的最小二乘均值差异为1.1（95%CI，0.41 - 1.79）（P = 0.002）。流鼻涕（10%）和黏膜颜色改变（9%）是鼻腔检查中最常见的发现，恶心和头晕是最常见的与治疗相关的不良事件。1例严重不良事件（即呼吸抑制）被认为与INFS有关。