静脉用槲寄生提取物治疗晚期癌症的 I 期临床试验。
Phase I Trial of Intravenous Mistletoe Extract in Advanced Cancer.
机构信息
The Sidney Kimmel Comprehensive Cancer Center, Johns Hopkins University School of Medicine, Baltimore, Maryland.
Department of Epidemiology, Johns Hopkins Bloomberg School of Public Health, Baltimore, Maryland.
出版信息
Cancer Res Commun. 2023 Feb 28;3(2):338-346. doi: 10.1158/2767-9764.CRC-23-0002. eCollection 2023 Feb.
PURPOSE
Mistletoe extract (ME) is widely used for patients with cancer to support therapy and to improve quality of life (QoL). However, its use is controversial due to suboptimal trials and a lack of data supporting its intravenous administration.
MATERIALS AND METHODS
This phase I trial of intravenous mistletoe (Helixor M) aimed to determine the recommended phase II dosing and to evaluate safety. Patients with solid tumor progressing on at least one line of chemotherapy received escalating doses of Helixor M three times a week. Assessments were also made of tumor marker kinetics and QoL.
RESULTS
Twenty-one patients were recruited. The median follow-up duration was 15.3 weeks. The MTD was 600 mg. Treatment-related adverse events (AE) occurred in 13 patients (61.9%), with the most common being fatigue (28.6%), nausea (9.5%), and chills (9.5%). Grade 3+ treatment-related AEs were noted in 3 patients (14.8%). Stable disease was observed in 5 patients who had one to six prior therapies. Reductions in baseline target lesions were observed in 3 patients who had two to six prior therapies. Objective responses were not observed. The disease control rate (percentage of complete/partial response and stable disease) was 23.8%. The median stable disease was 15 weeks. Serum cancer antigen-125 or carcinoembryonic antigen showed a slower rate of increase at higher dose levels. The median QoL by Functional Assessment of Cancer Therapy-General increased from 79.7 at week 1 to 93 at week 4.
CONCLUSIONS
Intravenous mistletoe demonstrated manageable toxicities with disease control and improved QoL in a heavily pretreated solid tumor population. Future phase II trials are warranted.
SIGNIFICANCE
Although ME is widely used for cancers, its efficacy and safety are uncertain. This first phase I trial of intravenous mistletoe (Helixor M) aimed to determine phase II dosing and to evaluate safety. We recruited 21 patients with relapsed/refractory metastatic solid tumor. Intravenous mistletoe (600 mg, 3/week) demonstrated manageable toxicities (fatigue, nausea, and chills) with disease control and improved QoL. Future research can examine ME's effect on survival and chemotherapy tolerability.
目的
槲寄生提取物(ME)被广泛用于癌症患者,以支持治疗并提高生活质量(QoL)。然而,由于试验效果不佳且缺乏支持其静脉给药的数据,其使用仍存在争议。
材料和方法
本研究为一项 I 期临床试验,旨在确定静脉用槲寄生(Helixor M)的 II 期推荐剂量,并评估其安全性。在至少一种化疗方案进展的实体瘤患者中,每周 3 次给予递增剂量的 Helixor M。还评估了肿瘤标志物动力学和 QoL。
结果
共招募了 21 名患者。中位随访时间为 15.3 周。最大耐受剂量为 600mg。13 名患者(61.9%)发生与治疗相关的不良事件(AE),最常见的是乏力(28.6%)、恶心(9.5%)和寒战(9.5%)。3 名患者(14.8%)发生 3 级及以上治疗相关 AE。5 名患者在既往治疗中接受了 1-6 种治疗方案,观察到疾病稳定。在既往接受了 2-6 种治疗方案的 3 名患者中观察到基线靶病灶减少。未观察到客观缓解。疾病控制率(完全/部分缓解和疾病稳定的百分比)为 23.8%。中位疾病稳定时间为 15 周。血清癌抗原 125 或癌胚抗原在较高剂量水平时显示出增加速度较慢。功能性评估癌症治疗-一般的生活质量中位数从第 1 周的 79.7 分增加到第 4 周的 93 分。
结论
静脉用槲寄生在既往治疗过的实体瘤患者中表现出可控的毒性、疾病控制和改善的生活质量。未来需要进行 II 期临床试验。
意义
尽管 ME 广泛用于癌症,但疗效和安全性尚不确定。本项首次关于静脉用槲寄生(Helixor M)的 I 期临床试验旨在确定 II 期剂量并评估安全性。我们招募了 21 名复发/难治性转移性实体瘤患者。静脉用槲寄生(600mg,每周 3 次)表现出可控的毒性(乏力、恶心和寒战)、疾病控制和改善的生活质量。未来的研究可以检验 ME 对生存和化疗耐受性的影响。
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