Department of Oncology, St. Jude Children's Research Hospital, Memphis, Tennessee.
Department of Pharmaceutical Sciences, St. Jude Children's Research Hospital, Memphis, Tennessee.
Clin Cancer Res. 2022 Jun 13;28(12):2536-2546. doi: 10.1158/1078-0432.CCR-21-4450.
To evaluate the safety, activity, and emergence of FLT3-kinase domain (KD) mutations with combination therapy of crenolanib and sorafenib in acute myeloid leukemia (AML) with FLT3-internal tandem duplication (ITD).
After in vitro and xenograft efficacy studies using AML cell lines that have FLT3-ITD with or without FLT3-KD mutation, a pilot study was performed with crenolanib (67 mg/m2/dose, three times per day on days 1-28) and two dose levels of sorafenib (150 and 200 mg/m2/day on days 8-28) in 9 pediatric patients with refractory/relapsed FLT3-ITD-positive AML. Pharmacokinetic, pharmacodynamic, and FLT3-KD mutation analysis were done in both preclinical and clinical studies.
The combination of crenolanib and sorafenib in preclinical models showed synergy without affecting pharmacokinetics of each agent, inhibited p-STAT5 and p-ERK for up to 8 hours, and led to significantly better leukemia response (P < 0.005) and survival (P < 0.05) compared with single agents. Fewer FLT3-KD mutations emerged with dose-intensive crenolanib (twice daily) and low-intensity sorafenib (three times/week) compared with daily crenolanib or sorafenib (P < 0.05). The crenolanib and sorafenib combination was tolerable without dose-limiting toxicities, and three complete remissions (one with incomplete count recovery) and one partial remission were observed in 8 evaluable patients. Median crenolanib apparent clearance showed a nonsignificant decrease during treatment (45.0, 40.5, and 20.3 L/hour/m2 on days 1, 7, and 14, respectively) without drug-drug interaction. Only 1 patient developed a FLT3-KD mutation (FLT3 F691L).
The combination of crenolanib and sorafenib was tolerable with antileukemic activities and rare emergence of FLT3-TKD mutations, which warrants further investigation.
评估克立硼罗联合索拉非尼治疗伴有 FLT3 内部串联重复(ITD)的急性髓系白血病(AML)患者中 FLT3 激酶结构域(KD)突变的安全性、活性和出现情况。
在使用具有或不具有 FLT3-KD 突变的 AML 细胞系进行体外和异种移植功效研究后,对 9 例难治/复发的 FLT3-ITD 阳性 AML 儿科患者进行了克立硼罗(67mg/m2/剂量,每日 3 次,第 1-28 天)和两个索拉非尼剂量水平(第 8-28 天每日 150mg/m2 和 200mg/m2)的试验性研究。在临床前和临床研究中均进行了药代动力学、药效学和 FLT3-KD 突变分析。
在临床前模型中,克立硼罗联合索拉非尼联合使用具有协同作用,且不影响每种药物的药代动力学,可抑制 p-STAT5 和 p-ERK 长达 8 小时,并导致明显更好的白血病反应(P<0.005)和生存(P<0.05)与单药治疗相比。与每日使用克立硼罗或索拉非尼相比,密集剂量的克立硼罗(每日两次)和低强度的索拉非尼(每周三次)可减少 FLT3-KD 突变的出现(P<0.05)。克立硼罗联合索拉非尼治疗耐受性良好,无剂量限制性毒性,在 8 例可评估患者中观察到 3 例完全缓解(1 例伴有不完全计数恢复)和 1 例部分缓解。在没有药物相互作用的情况下,克立硼罗的表观清除率在治疗期间呈非显著性下降(分别为第 1、7 和 14 天的 45.0、40.5 和 20.3L/hour/m2)。仅 1 例患者出现 FLT3-KD 突变(FLT3 F691L)。
克立硼罗联合索拉非尼治疗具有抗白血病活性且罕见出现 FLT3-TKD 突变,具有进一步研究的潜力。