伊布替尼用于复发/难治性慢性淋巴细胞白血病:英国和爱尔兰315例患者的疗效分析。
Ibrutinib for relapsed/refractory chronic lymphocytic leukemia: a UK and Ireland analysis of outcomes in 315 patients.
出版信息
Haematologica. 2016 Dec;101(12):1563-1572. doi: 10.3324/haematol.2016.147900. Epub 2016 Oct 18.
In 2014, ibrutinib was made available for relapsed/refractory chronic lymphocytic leukemia patients. The UK Chronic Lymphocytic Leukaemia Forum collected data from UK/Ireland patients with a minimum of 1 year follow-up with pre-planned primary endpoints; the number of patients still on therapy at 1 year "discontinuation-free survival" and 1 year overall survival. With a median of 16 months follow up, data on 315 patients demonstrated a 1 year discontinuation-free survival of 73.7% and a 1 year overall survival of 83.8%. Patients with better pre-treatment performance status (0/1 vs. 2+) had superior discontinuation-free survival (77.5% vs. 61.3%; P<0.0001) and overall survival (86.3% vs. 76.0%; P=0.0001). In univariable analysis, overall survival and discontinuation-free survival were not associated with the number of prior lines of therapy or 17p deletion. However, multivariable analysis identified an interaction between prior lines of therapy, age and 17p deletion, suggesting that older patients with 17p deletion did worse when treated with ibrutinib beyond the second line. Overall, 55.6% of patients had no first year dose reductions or treatment breaks of >14 days and had an overall survival rate of 89.7%, while 26% of patients had dose reductions and 13% had temporary treatment breaks of >14 days. We could not demonstrate a detrimental effect of dose reductions alone (1 year overall survival: 91.7%), but patients who had first year treatment breaks of >14 days, particularly permanent cessation of ibrutinib had both reduced 1 year overall survival (68.5%), and also a statistically significant excess mortality rate beyond one year. Although outcomes appear inferior to the RESONATE trial (1 year overall survival; 90%: progression-free survival; 84%), this may partly reflect the inclusion of performance status 2+ patients, and that 17.5% of patients permanently discontinued ibrutinib due to an event other than disease progression.
2014年,依鲁替尼开始用于复发/难治性慢性淋巴细胞白血病患者。英国慢性淋巴细胞白血病论坛收集了来自英国/爱尔兰患者的数据,这些患者至少随访1年,有预先设定的主要终点;1年“无停药生存期”和1年总生存期时仍在接受治疗的患者数量。中位随访16个月时,315例患者的数据显示1年无停药生存期为73.7%,1年总生存期为83.8%。治疗前体能状态较好(0/1对比2+)的患者无停药生存期更优(77.5%对比61.3%;P<0.0001),总生存期也更优(86.3%对比76.0%;P=0.0001)。单变量分析中,总生存期和无停药生存期与既往治疗线数或17p缺失无关。然而,多变量分析确定了既往治疗线数、年龄和17p缺失之间存在相互作用,表明17p缺失的老年患者在二线以上接受依鲁替尼治疗时情况更差。总体而言,55.6%的患者在第一年没有剂量减少或治疗中断超过14天,总生存率为89.7%,而26%的患者有剂量减少,13%的患者有超过14天的临时治疗中断。我们无法证明单独的剂量减少有有害影响(1年总生存期:91.7%),但在第一年有超过14天治疗中断的患者,尤其是永久停用依鲁替尼的患者,1年总生存期降低(68.5%),并且1年后有统计学上显著更高的死亡率。尽管结果似乎不如RESONATE试验(1年总生存期;90%:无进展生存期;84%),但这可能部分反映了纳入了体能状态为2+的患者,以及17.5%的患者由于疾病进展以外的事件永久停用了依鲁替尼。
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