曲美替尼和低剂量达拉非尼治疗晚期、既往治疗的野生型黑色素瘤的 II 期临床试验(TraMel-WT)。
Phase II Clinical Trial of Trametinib and Low-Dose Dabrafenib in Advanced, Previously Treated Wild-Type Melanoma (TraMel-WT).
机构信息
Department of Medical Oncology, Vrije Universiteit Brussel/Universitair Ziekenhuis Brussel, Brussels, Belgium.
Department of Ophthalmology, Vrije Universiteit Brussel/Universitair Ziekenhuis Brussel, Brussels, Belgium.
出版信息
JCO Precis Oncol. 2024 Oct;8:e2300493. doi: 10.1200/PO.23.00493. Epub 2024 Feb 14.
PURPOSE
Patients with / wild-type melanoma who progress after immune checkpoint inhibitors (ICIs) have a poor prognosis. MEK inhibition has shown activity in this patient population but is associated with treatment-limiting skin toxicity. Combining a BRAF inhibitor with a MEK inhibitor is associated with less skin toxicity.
METHODS
This phase II trial investigated trametinib (2 mg once daily) in patients with advanced / wild-type, ICI-refractory melanoma. In case of treatment-limiting skin toxicity, low-dose dabrafenib (50 mg twice daily) was added to trametinib. After a trial amendment, both drugs were combined up-front. The confirmed objective response rate (cORR) served as the primary end point.
RESULTS
Twenty-four patients were included (50% male; median age 57 years; 92% Eastern Cooperative Oncology Group Performance Status 0-2; 75% stage IV-M1c/stage IV-M1d; median number of prior therapies: two [range, 1-5]). Three patients were enrolled before and 21 patients after the amendment, respectively. Seven confirmed and one unconfirmed partial responses (PRs) were observed (cORR, 29.2%). The median duration of response was 16.6 weeks (95% CI, 5.5 to 27.7). Stable disease (SD) was the best response in an additional five patients. Among the responding patients, genetic alterations causing mitogen-activated protein kinase (MAPK) pathway activation were documented in six patients. The disease control rate in patients with MAPK pathway-activating alterations was 64.3% (five confirmed PR, one unconfirmed PR, and three SD). The median progression-free survival was 13.3 weeks (95% CI, 3.5 to 23.1), and the median overall survival was 54.3 weeks (95% CI, 37.9 to 70.6). Adding low-dose dabrafenib to trametinib effectively mitigated or prevented treatment-limiting trametinib-related skin toxicity.
CONCLUSION
The combination of trametinib plus low-dose dabrafenib demonstrated encouraging efficacy and effective mitigation of skin toxicity in patients with advanced, ICI-pretreated / wild-type melanoma patients. MAPK pathway-activating alterations hold promise as a predictive biomarker.
目的
接受免疫检查点抑制剂(ICI)治疗后进展的 / 野生型黑色素瘤患者预后较差。MEK 抑制在这部分患者中显示出疗效,但与治疗相关的皮肤毒性相关。BRAF 抑制剂联合 MEK 抑制剂与较少的皮肤毒性相关。
方法
本 II 期试验研究了曲美替尼(2mg 每日一次)在晚期 / 野生型、ICI 难治性黑色素瘤患者中的应用。在出现治疗相关的皮肤毒性时,曲美替尼加用低剂量达拉非尼(50mg 每日两次)。在试验修订后,两种药物均联合应用。确认的客观缓解率(cORR)作为主要终点。
结果
共纳入 24 例患者(50%为男性;中位年龄 57 岁;92%东部肿瘤协作组体力状态 0-2 分;75%为 IV-M1c/IV-M1d 期;中位治疗线数为 2 条[范围,1-5 条])。分别有 3 例患者在修订前和 21 例患者在修订后入组。观察到 7 例确认和 1 例未确认的部分缓解(cORR 为 29.2%)。缓解持续时间的中位数为 16.6 周(95%CI,5.5-27.7)。另外 5 例患者的最佳反应为疾病稳定(SD)。在缓解的患者中,有 6 例患者记录到导致丝裂原活化蛋白激酶(MAPK)通路激活的遗传改变。MAPK 通路激活改变患者的疾病控制率为 64.3%(5 例确认的部分缓解,1 例未确认的部分缓解和 3 例 SD)。无进展生存期的中位数为 13.3 周(95%CI,3.5-23.1),总生存期的中位数为 54.3 周(95%CI,37.9-70.6)。曲美替尼联合低剂量达拉非尼可有效减轻或预防治疗相关的曲美替尼相关皮肤毒性。
结论
曲美替尼联合低剂量达拉非尼在晚期、ICI 预处理 / 野生型黑色素瘤患者中显示出令人鼓舞的疗效和有效的皮肤毒性缓解。MAPK 通路激活改变有望成为预测生物标志物。
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