Cancer Treatment Centers of America, Comprehensive Care and Research Center, Chicago, IL, USA.
NRG Oncology Statistics and Data Management Center, Roswell Park Comprehensive Cancer Center, Buffalo, NY, USA.
Gynecol Oncol. 2020 Aug;158(2):354-360. doi: 10.1016/j.ygyno.2020.05.013. Epub 2020 May 24.
Methotrexate and actinomycin-D are both effective first-line drugs for low-risk (WHO score 0-6) Gestational Trophoblastic Neoplasia (GTN) with considerable debate about which is more effective, less toxic, and better tolerated. The primary trial objective was to test if treatment with multi-day methotrexate (MTX) was inferior to pulse actinomycin-D (ACT-D). Secondary objectives included evaluation of severity and frequency of adverse events, and impact on quality of life (QOL).
This was a prospective international cooperative group randomized phase III two arm non-inferiority study (Clinical Trials Identifier: (NCT01535053). The control arm was ACT-D; the experimental arm was multi-day MTX regimen (institutional preference of 5 or 8 day). Outcome measures included complete response rate, recurrence rate, toxicity, and QOL as measured by FACT-G and FACIT supplemental items.
The complete response rates for multi-day methotrexate and pulse actinomycin-D were 88% (23/26 patients) and 79% (22/28 patients) (p = NS) respectively, there were two recurrences in each arm, and 100% of patients survived. Significant toxicity was minimal, but mouth sores (mucositis), and eye pain were significantly more common in the MTX arm (p = 0.001 and 0.01 respectively). Quality of life showed no significant difference in overall quality of life, body image, sexual function, or treatment related side effects. The study was closed for low accrual rate (target 384, actual accrual 57), precluding statistical analysis of the primary objective.
The complete response rate for multi-day methotrexate was higher than actinomycin-D, but did not reach statistical significance. The multi-day MTX regimens were associated with significantly more mucositis and were significantly less convenient.
甲氨蝶呤和放线菌素 D 均为低危(WHO 评分 0-6)妊娠滋养细胞肿瘤(GTN)的有效一线药物,对于哪种药物更有效、毒性更小、耐受性更好,存在较大争议。主要试验目的是检测多日甲氨蝶呤(MTX)治疗是否劣于脉冲放线菌素 D(ACT-D)。次要目标包括评估不良反应的严重程度和频率,以及对生活质量(QOL)的影响。
这是一项前瞻性国际合作组随机 III 期双臂非劣效性研究(临床试验标识符:(NCT01535053)。对照组为 ACT-D;实验组为多日 MTX 方案(机构偏好 5 或 8 天)。结局指标包括完全缓解率、复发率、毒性和 QOL,分别采用 FACT-G 和 FACIT 补充项目进行评估。
多日 MTX 和脉冲 ACT-D 的完全缓解率分别为 88%(23/26 例患者)和 79%(22/28 例患者)(p=NS),两组各有 2 例复发,所有患者均存活。显著毒性最小,但口腔疼痛(黏膜炎)和眼痛在 MTX 组更为常见(p=0.001 和 0.01)。生活质量在总体生活质量、身体形象、性功能或与治疗相关的副作用方面无显著差异。由于入组率低(目标 384 例,实际入组 57 例),该研究提前关闭,无法对主要结局进行统计学分析。
多日 MTX 的完全缓解率高于 ACT-D,但未达到统计学意义。多日 MTX 方案与显著更高的黏膜炎发生率相关,且便利性显著降低。
