Robert H Lurie Comprehensive Cancer Center, Northwestern University, Chicago, IL, USA.
Abramson Comprehensive Cancer Center, University of Pennsylvania, Philadelphia, PA, USA.
Cancer Med. 2021 Feb;10(3):797-805. doi: 10.1002/cam4.3652. Epub 2020 Dec 19.
The FLT3 inhibitor gilteritinib has clinical activity in patients with FLT3-mutated (FLT3 ) relapsed/refractory (R/R) acute myeloid leukemia (AML). The impact of FLT3 mutation clearance and the achievement of composite complete remission (CRc) and complete remission/complete remission with partial hematologic recovery (CR/CRh) on overall survival (OS) in patients with FLT3 R/R AML treated with single-agent gilteritinib in a phase 1/2 trial were evaluated. Using next-generation sequencing, a FLT3-ITD variant allele frequency of ≤10 was used to define FLT3-ITD clearance in patients with no morphologic leukemia (ie, CRc). A total of 108 patients with FLT3-ITD-positive (FLT3-ITD+) R/R AML were analyzed; 95 of these patients had received ≥80-mg/day gilteritinib. Ten of the 95 patients had FLT3-ITD clearance; eight of these 10 patients achieved CRc and were considered negative for measurable residual disease. There was a trend toward longer OS in patients who attained CRc with FLT3-ITD clearance (131.4 weeks) versus those who achieved CRc and did not have FLT3-ITD clearance (n = 41; 43.3 weeks; HR = 0.416; p = 0.066). Among patients treated with ≥80-mg/day gilteritinib who achieved CR/CRh (n = 24), seven had FLT3-ITD clearance. Among patients who received 120-mg/day gilteritinib, those who achieved CR/CRh had a longer median OS (70.6 weeks) and higher 52-week survival probability (66.7%) than patients who did not achieve CR/CRh (n = 71; median OS, 41.7 weeks; 52-week survival probability, 20.2%). Overall, these data suggest that gilteritinib can induce deep molecular responses in patients with FLT3-ITD+ R/R AML, and in the setting of CRc or CR/CRh, these responses may be associated with prolonged survival.
FLT3 抑制剂吉特替尼在 FLT3 突变(FLT3 )复发/难治性(R/R)急性髓系白血病(AML)患者中具有临床活性。在一项 1/2 期试验中,评估了单药吉特替尼治疗 FLT3 R/R AML 患者中 FLT3 突变清除率以及复合完全缓解(CRc)和完全缓解/完全缓解伴部分血液学恢复(CR/CRh)对总生存期(OS)的影响。使用下一代测序,无形态白血病(即 CRc)患者中使用≤10 的 FLT3-ITD 变异等位基因频率来定义 FLT3-ITD 清除率。共分析了 108 例 FLT3-ITD 阳性(FLT3-ITD+)R/R AML 患者;其中 95 例患者接受了≥80mg/天的吉特替尼治疗。在 95 例患者中有 10 例达到了 FLT3-ITD 清除;这 10 例患者中有 8 例达到了 CRc,并且被认为无可测量残留疾病。在达到 CRc 且 FLT3-ITD 清除的患者中,OS 较长(131.4 周),而达到 CRc 且未达到 FLT3-ITD 清除的患者中,OS 较长(n=41;43.3 周;HR=0.416;p=0.066)。在接受≥80mg/天吉特替尼治疗且达到 CR/CRh 的患者(n=24)中,有 7 例达到了 FLT3-ITD 清除。在接受 120mg/天吉特替尼治疗的患者中,达到 CR/CRh 的患者的中位 OS 更长(70.6 周),52 周生存率更高(66.7%),而未达到 CR/CRh 的患者(n=71;中位 OS,41.7 周;52 周生存率,20.2%)。总的来说,这些数据表明,吉特替尼可以诱导 FLT3-ITD+ R/R AML 患者的深度分子反应,并且在 CRc 或 CR/CRh 的情况下,这些反应可能与延长生存相关。
