Hagen Neil A, Cantin Lyne, Constant John, Haller Tina, Blaise Gilbert, Ong-Lam May, du Souich Patrick, Korz Walter, Lapointe Bernard
Tom Baker Cancer Centre and Division of Palliative Medicine, University of Calgary, 1331 29 Street NW, Calgary, AB, Canada T2N4N2.
ClinForce Services Inc., Vancouver, BC, Canada.
Pain Res Manag. 2017;2017:7212713. doi: 10.1155/2017/7212713. Epub 2017 May 7.
This study evaluated subcutaneous injections of tetrodotoxin (TTX) for the treatment of moderate to severe, inadequately controlled cancer-related pain.
Eligible patients were randomized to receive TTX (30 g) or placebo subcutaneously twice daily for four consecutive days. Efficacy was assessed using pain and composite endpoints (including pain and quality of life measures), and safety was evaluated using standard measures.
165 patients were enrolled at 19 sites in Canada, Australia, and New Zealand, with 149 patients in the primary analysis "intent-to-treat" population. The primary analysis supports a clinical benefit of TTX over placebo based on the pain endpoint alone with a clinically significant estimated effect size of 16.2% ( = 0.0460). The value was nominally statistically significant after prespecified (Bonferroni Holm) adjustment for the two primary endpoints but not at the prespecified two-sided 5% level. The mean duration of analgesic response was 56.7 days (TTX) and 9.9 days (placebo). Most common adverse events were nausea, dizziness, and oral numbness or tingling and were generally mild to moderate and transient.
Although underpowered, this study demonstrates a clinically important analgesic signal. TTX may provide clinically meaningful analgesia for patients who have persistent moderate to severe cancer pain despite best analgesic care. This clinical study is registered with ClinicalTrials.gov (NCT00725114).
本研究评估皮下注射河豚毒素(TTX)治疗中度至重度、控制不佳的癌症相关疼痛的效果。
符合条件的患者被随机分组,连续四天每天两次皮下注射TTX(30μg)或安慰剂。使用疼痛和综合终点指标(包括疼痛和生活质量测量)评估疗效,使用标准测量方法评估安全性。
在加拿大、澳大利亚和新西兰的19个地点招募了165名患者,149名患者纳入主要分析的“意向性治疗”人群。主要分析表明,仅基于疼痛终点,TTX比安慰剂具有临床益处,估计效应大小为16.2%,具有临床显著性(P = 0.0460)。对两个主要终点进行预先指定的(Bonferroni Holm)调整后,P值名义上具有统计学显著性,但未达到预先指定的双侧5%水平。镇痛反应的平均持续时间为TTX组56.7天,安慰剂组9.9天。最常见的不良事件是恶心、头晕、口腔麻木或刺痛,一般为轻至中度且短暂。
尽管样本量不足,但本研究显示出具有临床重要意义的镇痛信号。对于尽管接受了最佳镇痛治疗仍持续存在中度至重度癌症疼痛的患者,TTX可能提供具有临床意义的镇痛效果。本临床研究已在ClinicalTrials.gov注册(NCT00725114)。
