SPIRE 研究:DNA 甲基转移酶抑制剂地西他滨联合顺铂和吉西他滨治疗实体瘤包括尿路上皮癌的 I 期临床研究
Phase I Trial of DNA Methyltransferase Inhibitor Guadecitabine Combined with Cisplatin and Gemcitabine for Solid Malignancies Including Urothelial Carcinoma (SPIRE).
机构信息
Southampton Clinical Trials Unit, University of Southampton, Southampton, England, United Kingdom.
University Hospital Southampton NHS Foundation Trust, Southampton, England, United Kingdom.
出版信息
Clin Cancer Res. 2021 Apr 1;27(7):1882-1892. doi: 10.1158/1078-0432.CCR-20-3946. Epub 2021 Jan 20.
PURPOSE
Preclinical data indicate that DNA methyltransferase inhibition will circumvent cisplatin resistance in various cancers.
PATIENT AND METHODS
SPIRE comprised a dose-escalation phase for incurable metastatic solid cancers, followed by a randomized dose expansion phase for neoadjuvant treatment of T2-4a N0 M0 bladder urothelial carcinoma. The primary objective was a recommended phase II dose (RP2D) for guadecitabine combined with gemcitabine and cisplatin. Treatment comprised 21-day gemcitabine and cisplatin cycles (cisplatin 70 mg/m, i.v., day 8 and gemcitabine 1,000 mg/m, i.v., days 8 + 15). Guadecitabine was injected subcutaneously on days 1-5, within escalation phase cohorts, and to half of 20 patients in the expansion phase. Registration ID: ISRCTN 16332228.
RESULTS
Within the escalation phase, dose-limiting toxicities related predominantly to myelosuppression requiring G-CSF prophylaxis from cohort 2 (guadecitabine 20 mg/m, days 1-5). The most common grade ≥3 adverse events in 17 patients in the dose-escalation phase were neutropenia (76.5%), thrombocytopenia (64.7%), leukopenia (29.4%), and anemia (29.4%). Addition of guadecitabine to gemcitabine and cisplatin in the expansion phase resulted in similar rates of severe hematologic adverse events, similar cisplatin dose intensity, but modestly reduced gemcitabine dose intensity. Radical treatment options after chemotherapy were not compromised. Pharmacodynamics evaluations indicated guadecitabine maximal target effect at the point of cisplatin administration. Pharmacokinetics were consistent with prior data. No treatment-related deaths occurred.
CONCLUSIONS
The guadecitabine RP2D was 20 mg/m, days 1-5, in combination with gemcitabine and cisplatin and required GCSF prophylaxis. Gene promoter methylation pharmacodynamics are optimal with this schedule. Addition of guadecitabine to gemcitabine and cisplatin was tolerable, despite some additional myelosuppression, and warrants further investigation to assess efficacy.
目的
临床前数据表明,DNA 甲基转移酶抑制可规避多种癌症的顺铂耐药性。
患者和方法
SPIRE 包括不可治愈的转移性实体瘤的剂量递增阶段,随后是新辅助治疗 T2-4a N0 M0 膀胱尿路上皮癌的随机剂量扩展阶段。主要目标是确定吉西他滨联合吉西他滨和顺铂的推荐 II 期剂量(RP2D)。治疗包括 21 天的吉西他滨和顺铂周期(顺铂 70mg/m,静脉注射,第 8 天和吉西他滨 1000mg/m,静脉注射,第 8 天+第 15 天)。在递增阶段的队列中,吉西他滨和顺铂周期内,以及扩展阶段的 20 名患者中的一半,皮下注射 Guadacitabine 第 1-5 天。注册号:ISRCTN16332228。
结果
在递增阶段,剂量限制毒性主要与需要 G-CSF 预防的骨髓抑制有关,这需要从第 2 队列(Guadecitabine 20mg/m,第 1-5 天)开始。在递增阶段的 17 名患者中,最常见的≥3 级不良事件是中性粒细胞减少症(76.5%)、血小板减少症(64.7%)、白细胞减少症(29.4%)和贫血(29.4%)。在扩展阶段,吉西他滨和顺铂联合 Guadacitabine 治疗导致严重血液学不良事件发生率相似、顺铂剂量强度相似,但吉西他滨剂量强度略有降低。化疗后根治性治疗方案不受影响。药效学评估表明 Guadacitabine 在给予顺铂时达到最大靶效应。药代动力学与先前的数据一致。无治疗相关死亡发生。
结论
Guadacitabine 的 RP2D 为 20mg/m,第 1-5 天,与吉西他滨和顺铂联合使用,需要 GCSF 预防。这种方案下基因启动子甲基化药效学最佳。尽管骨髓抑制略有增加,但 Guadacitabine 联合吉西他滨和顺铂治疗耐受性良好,值得进一步研究以评估疗效。
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