Department of Medicine, Sarcoma Medical Oncology Service, Memorial Sloan Kettering Cancer Center (MSKCC), 1275 York Avenue, New York, NY, 10065, USA.
Weill Cornell Medical College, New York, NY, USA.
Invest New Drugs. 2019 Apr;37(2):282-290. doi: 10.1007/s10637-018-0648-z. Epub 2018 Aug 13.
Background Preclinical studies suggest that imatinib resistance in gastrointestinal stromal tumor (GIST) can be mediated by MAP-kinase activation via fibroblast growth factor (FGF) signaling. In FGF stimulated GIST cell lines, BGJ398, a pan-FGFR kinase inhibitor in combination with imatinib, was cytotoxic and superior to imatinib therapy alone. In FGF-dependent GIST, the combination of BGJ398 and imatinib may provide a mechanism to overcome imatinib resistance. Methods This phase Ib study of BGJ398 and imatinib was performed in patients with imatinib refractory advanced GIST. A standard 3 + 3 dosing schema was utilized to determine the recommended phase II dose (RP2D). Two treatment schedules were evaluated incorporating imatinib 400 mg daily in combination with (A) BGJ398 daily 3 weeks on, 1 week off or (B) BGJ398 daily 1 week on, 3 weeks off. Results 16 patients enrolled. The median age was 54 years (range: 44-77), 81% were male, and the median number of lines of prior therapy was 4 [range: 2-6, 13 patients had ≥3 prior therapies]. 12 patients received treatment on schedule A [BGJ398 dose range: 25 - 75 mg]: 2 patients experienced dose limiting toxicities (DLT) (n = 1, myocardial infarction & grade (G)4 CPK elevation; n = 1, G3 ALT elevation) on schedule A (BGJ398 75 mg), significant hyperphosphatemia, an on-target effect, was not observed, implying the maximum tolerated dose was below the therapeutic dose. Following protocol amendment, 4 patients enrolled on schedule B [BGJ398 dose range: 75 - 100 mg]: no DLTs were observed. The most common treatment related adverse events occurring in >15% of patients included CPK elevation (50%), lipase elevation (44%), hyperphosphatemia (24%), anemia (19%), and peripheral edema (19%). Among the 12 evaluable patients, stable disease (SD) was the best response observed in 7 patients by RECIST v1.1 and 9 patients by CHOI. Stable disease ≥ 32 weeks was observed in 3 patients (25%). Median progression free survival was 12.1 weeks (95% CI 4.7-19.5 weeks). Conclusions Toxicity was encountered with the combination therapy of BGJ398 and imatinib. Due to withdrawal of sponsor support the study closed before the RP2D or dosing schedule of the combination therapy was identified. In heavily pre-treated patients, stable disease ≥ 32 weeks was observed in 3 of 12 evaluable patients. Trial Registration: NCT02257541 .
临床前研究表明,成纤维细胞生长因子(FGF)信号通路介导的丝裂原活化蛋白激酶(MAPK)激活可导致胃肠道间质瘤(GIST)对伊马替尼产生耐药。在 FGF 刺激的 GIST 细胞系中,泛 FGFR 激酶抑制剂 BGJ398 联合伊马替尼具有细胞毒性,且优于单独使用伊马替尼的治疗效果。在 FGF 依赖性 GIST 中,BGJ398 联合伊马替尼的组合可能为克服伊马替尼耐药提供一种机制。
这项针对伊马替尼难治性晚期 GIST 患者的 BGJ398 和伊马替尼的 Ib 期研究采用了标准的 3+3 剂量递增方案来确定推荐的 II 期剂量(RP2D)。评估了两种治疗方案,方案 A 为每日给予伊马替尼 400mg 联合 BGJ398,用药方案为 3 周用药、1 周停药;方案 B 为每日给予伊马替尼 400mg 联合 BGJ398,用药方案为 1 周用药、3 周停药。
共纳入 16 例患者。患者中位年龄为 54 岁(范围:44-77 岁),81%为男性,中位既往治疗线数为 4 条(范围:2-6 条,13 例患者有≥3 条既往治疗线)。12 例患者按计划 A(BGJ398 剂量范围:25-75mg)接受治疗:2 例患者出现剂量限制性毒性(DLT)(n=1,心肌梗死和 CPK 升高 G4;n=1,ALT 升高 G3),计划 A(BGJ398 75mg)时观察到显著高磷血症,这是一种靶标效应,表明最大耐受剂量低于治疗剂量。方案修订后,4 例患者按计划 B(BGJ398 剂量范围:75-100mg)接受治疗:未观察到 DLT。>15%的患者中最常见的与治疗相关的不良事件包括 CPK 升高(50%)、脂肪酶升高(44%)、高磷血症(24%)、贫血(19%)和外周水肿(19%)。在 12 例可评估的患者中,根据 RECIST v1.1,7 例患者和根据 CHOI,9 例患者观察到最佳疾病控制为疾病稳定(SD)。3 例患者(25%)观察到 SD 持续时间≥32 周。中位无进展生存期为 12.1 周(95%CI:4.7-19.5 周)。
BGJ398 和伊马替尼联合治疗时出现毒性。由于赞助商支持的撤回,在确定 RP2D 或联合治疗的剂量方案之前,该研究提前关闭。在经过大量预处理的患者中,12 例可评估患者中有 3 例观察到 SD 持续时间≥32 周。
NCT02257541。
