Baccarani Michele, Druker Brian J, Branford Susan, Kim Dong-Wook, Pane Fabrizio, Mongay Lidia, Mone Manisha, Ortmann Christine-Elke, Kantarjian Hagop M, Radich Jerald P, Hughes Timothy P, Cortes Jorge E, Guilhot François
Int J Hematol. 2014;99(5):616-24. doi: 10.1007/s12185-014-1566-2.
The TOPS trial evaluated high- (800 mg/day; n = 319) versus standard-dose (400 mg/day; n = 157) imatinib in patients newly diagnosed with Philadelphia chromosome-positive chronic myeloid leukemia in chronic phase. Patients had a minimum follow-up of 42 months or discontinued early. Major molecular response (MMR) rates were similar between arms at (51.6 vs 50.2 % for 400 and 800 mg/day, respectively; P = 0.77) and by (75.8 vs 79.0 %; P = 0.4807) 42 months. There were no differences in event-free survival (EFS), progression-free survival(PFS), or overall survival (OS) between arms. The estimated rates of PFS on treatment and OS at 42 months were significantly higher in patients with MMR at 6, 12, and 18 months compared with those without MMR.Adverse events were more frequent with high-dose imatinib. Patients with B1 treatment interruption (vs [1) and those able to maintain imatinib C600 mg/day (vs\600 mg/day) in the first year of treatment had faster and higher response rates, but no improvement in EFS or PFS. Adherence to prescribed dose without interruption may be more important than initiation of therapy with higher doses of imatinib. Achievement of MMR correlated with longterm clinical outcomes.
TOPS试验评估了高剂量(800毫克/天;n = 319)与标准剂量(400毫克/天;n = 157)伊马替尼在新诊断的慢性期费城染色体阳性慢性髓性白血病患者中的疗效。患者的最短随访时间为42个月或提前停药。两组之间的主要分子反应(MMR)率相似(400毫克/天和800毫克/天分别为51.6%和50.2%;P = 0.77),到42个月时分别为(75.8%对79.0%;P = 0.4807)。两组之间的无事件生存期(EFS)、无进展生存期(PFS)或总生存期(OS)没有差异。在6、12和18个月达到MMR的患者,其42个月时的估计PFS率和OS率显著高于未达到MMR的患者。高剂量伊马替尼的不良事件更频繁。在治疗的第一年出现B1治疗中断(与未中断相比)以及能够维持伊马替尼剂量≥600毫克/天(与<600毫克/天相比)的患者,其反应率更快且更高,但EFS或PFS没有改善。坚持规定剂量不间断可能比开始使用更高剂量的伊马替尼治疗更重要。达到MMR与长期临床结果相关。
