Department of Hematology, Kuwait Cancer Control Center, Shuwaikh city, Kuwait.
Department of Leukemia, The University of Texas MD Anderson Cancer Center, Houston, Texas.
Am J Hematol. 2018 Jan;93(1):84-90. doi: 10.1002/ajh.24943. Epub 2017 Nov 9.
Additional cytogenetic abnormalities (ACA) are considered a high risk feature in chronic myeloid leukemia (CML). However, its prognostic significance at the time of diagnosis in the setting of new tyrosine kinase inhibitors (TKIs) is less well understood. Patients with CML in CP with or without ACA at diagnosis treated with frontline TKIs in prospective clinical trials were analyzed for outcomes. Among 603 patients treated, 29 (5%) had ACA. Patients with ACA included 2 of 72 (2.8%) treated with imatinib 400 mg, 9 of 207 (4.3%) with imatinib 800 mg, 10 of 148 (6.7%) with dasatinib, 6 of 126 (4.7%) with nilotinib, and 2 of 50 (4%) with ponatinib. There was a significantly higher rate of complete cytogenetic response (CCyR) at 6 months in patients without ACA (P = .02). However cumulative CCyR and major molecular response (MMR) rates were not different. Similarly, MR4.0 and MR4.5 rates were similar for both groups; two CML-ACA patients maintained MR 4.5 for at least 2 years. At 5 years, ACA at diagnosis did not significantly impact transformation-free, failure-free, event-free, or overall survival expectations. Acknowledging small sample size estimates, response rates and survival outcomes were comparable in CP with ACA irrespective of whether chromosomal abnormalities were "major route" or other. The presence of ACA at diagnosis does not confer worse prognosis for patients with CML treated with TKI. Thus, the presence of ACA at diagnosis should not alter treatment strategies in these patients.
附加细胞遗传学异常(ACA)被认为是慢性髓性白血病(CML)的高风险特征。然而,在新的酪氨酸激酶抑制剂(TKI)治疗背景下,其在诊断时的预后意义尚不清楚。分析了接受一线 TKI 治疗的伴有或不伴有 ACA 的 CML-CP 患者的结局。在 603 例接受治疗的患者中,29 例(5%)存在 ACA。ACA 患者包括 72 例中接受伊马替尼 400mg 治疗的 2 例(2.8%)、207 例中接受伊马替尼 800mg 治疗的 9 例(4.3%)、148 例中接受达沙替尼治疗的 10 例(6.7%)、126 例中接受尼洛替尼治疗的 6 例(4.7%)和 50 例中接受 ponatinib 治疗的 2 例(4%)。无 ACA 患者在 6 个月时完全细胞遗传学缓解(CCyR)率显著更高(P=.02)。然而,累积 CCyR 和主要分子缓解(MMR)率无差异。同样,两组的 MR4.0 和 MR4.5 率相似;两名 CML-ACA 患者至少保持 MR4.5 缓解 2 年。5 年时,诊断时的 ACA 并不显著影响无转化、无失败、无事件或总生存预期。尽管样本量估计较小,但 CP 中存在 ACA 的患者无论染色体异常是否为“主要途径”或其他,其反应率和生存结局均无差异。TKI 治疗的 CML 患者诊断时存在 ACA 并不会导致预后更差。因此,这些患者的治疗策略不应因 ACA 的存在而改变。
