一项评估 MEK 抑制剂 cobimetinib 联合 ERK1/2 抑制剂 GDC-0994 治疗晚期实体瘤患者的 Ib 期研究。
A Phase Ib Study to Evaluate the MEK Inhibitor Cobimetinib in Combination with the ERK1/2 Inhibitor GDC-0994 in Patients with Advanced Solid Tumors.
机构信息
Massachusetts General Hospital, Boston, Massachusetts, USA.
Division of Oncology, Washington University Medical School, St. Louis, Missouri, USA.
出版信息
Oncologist. 2020 Oct;25(10):833-e1438. doi: 10.1634/theoncologist.2020-0292. Epub 2020 May 28.
LESSONS LEARNED
Despite strong preclinical rationale, combined cobimetinib-mediated MEK inhibition and GDC-0994-mediated ERK inhibition was not tolerable on two 28-day dosing schedules in which GDC-0994 was given for 21 days continuously and cobimetinib administered over 21 days either continuously or intermittently. Adverse events were as expected for mitogen-activated protein kinase pathway inhibition, but overlapping and cumulative toxicities could not be managed on either dosing schedule. Pharmacokinetic parameters of cobimetinib and GDC-0994 given in combination were similar to those previously observed in monotherapy studies, so that there was no evidence of drug-drug interaction. Cycle 1 metabolic responses were observed by 18F-fluorodeoxyglucose-positron emission tomography but were not predictive of outcome measured by RECIST 1.1.
BACKGROUND
Simultaneous targeting of multiple nodes in the mitogen-activated protein kinase (MAPK) pathway offers the prospect of enhanced activity in RAS-RAF-mutant tumors. This phase Ib trial evaluated the combination of cobimetinib (MEK inhibitor) and GDC-0994 (ERK inhibitor) in patients with locally advanced or metastatic solid tumors.
METHODS
Cobimetinib and GDC-0994 were administered orally on two separate dosing schedules. Arm A consisted of concurrent cobimetinib and GDC-0994 once daily for 21 days of a 28-day cycle; Arm B consisted of intermittent dosing of cobimetinib on a 28-day cycle concurrent with GDC-0994 daily for 21 days of a 28-day cycle.
RESULTS
In total, 24 patients were enrolled. For Arm A, owing to cumulative grade 1-2 toxicity, the dose of cobimetinib was decreased. For Arm B, dose increases of GDC-0994 and cobimetinib were intolerable with grade 3 dose-limiting toxicities of myocardial infarction and rash. Pharmacokinetic data did not show evidence of a drug-drug interaction. Overall, seven patients had a best overall response of stable disease (SD) and one patient with pancreatic adenocarcinoma had an unconfirmed partial response.
CONCLUSION
The safety profile of MEK and ERK inhibition demonstrated classic MAPK inhibitor-related adverse events (AEs). However, overlapping AEs and cumulative toxicity could not be adequately managed on either dosing schedule, restricting the ability to further develop this combination.
经验教训
尽管具有强有力的临床前理论基础,但在两种 28 天给药方案中,联合使用 cobimetinib 介导的 MEK 抑制和 GDC-0994 介导的 ERK 抑制是不可耐受的,其中 GDC-0994 连续给药 21 天,而 cobimetinib 连续或间断给药 21 天。不良事件与丝裂原活化蛋白激酶(MAPK)途径抑制相符,但在两种给药方案中均不能有效管理重叠和累积毒性。联合使用 cobimetinib 和 GDC-0994 的药代动力学参数与单药研究中观察到的相似,因此没有证据表明存在药物相互作用。18F-氟脱氧葡萄糖正电子发射断层扫描(18F-FDG-PET)观察到了 1 个周期的代谢反应,但与 RECIST 1.1 测量的结果无关。
背景
同时靶向 MAPK 途径中的多个节点有望增强 RAS-RAF 突变肿瘤的活性。这项 Ib 期试验评估了 cobimetinib(MEK 抑制剂)和 GDC-0994(ERK 抑制剂)联合用于局部晚期或转移性实体瘤患者。
方法
cobimetinib 和 GDC-0994 分别在两种不同的剂量方案中口服给药。A 臂为连续 21 天的 28 天周期中每日同时给予 cobimetinib 和 GDC-0994;B 臂为连续 28 天周期中每日给予 GDC-0994 的同时,间断给予 cobimetinib,21 天为一个周期。
结果
总共入组了 24 名患者。由于累积的 1-2 级毒性,A 臂 cobimetinib 的剂量减少。对于 B 臂,GDC-0994 和 cobimetinib 的剂量增加不可耐受,导致 3 级剂量限制性毒性(心肌梗死和皮疹)。药代动力学数据未显示药物相互作用的证据。总的来说,7 名患者的最佳总体缓解为疾病稳定(SD),1 名胰腺腺癌患者的部分缓解未经确认。
结论
MEK 和 ERK 抑制的安全性特征显示出典型的 MAPK 抑制剂相关不良事件(AE)。然而,在两种给药方案中均不能有效管理重叠的 AE 和累积毒性,从而限制了进一步开发这种联合用药的能力。
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