马来西亚-新加坡 2010 年急性淋巴细胞白血病研究非高危组延迟强化期间成功降低毒性。
Successful toxicity reduction during delayed intensification in the non-high-risk arm of Malaysia-Singapore Acute Lymphoblastic Leukaemia 2010 study.
机构信息
Viva-University Children's Cancer Centre, Khoo Teck Puat-National University Children's Medical Institute, National University Hospital, National University Health System, Singapore; Department of Paediatrics, Yong Loo Lin School of Medicine, National University Singapore, Singapore.
Department of Paediatric Subspecialties Haematology/Oncology Service, KK Women's and Children's Hospital, Singapore.
出版信息
Eur J Cancer. 2021 Jan;142:92-101. doi: 10.1016/j.ejca.2020.10.010. Epub 2020 Nov 24.
UNLABELLED
In non-high-risk (non-HR) patients, the Malaysia-Singapore Acute Lymphoblastic Leukaemia 2003 (MS2003) study achieved good outcomes. However, its delayed-intensification (DI) phase, comprising repeated blocks of protocol III (2003-PIII), was toxic and caused significant treatment delays. The successor MS2010 study attempted to lower DI toxicity by replacing myelosuppressive drugs (doxorubicin, cytarabine) with vincristine and asparaginase.
PATIENTS AND METHODS
We analysed 1748 admissions for fever in 315 Singapore children with non-HR acute lymphoblastic leukaemia (ALL) (MS2003, n = 183; MS2010, n = 132), comprising 76% of the total cohort (n = 413), to study the impact of these changes.
RESULTS
The new 2010-PVa which has no doxorubicin, was associated with significantly fewer hospitalisations due to fever (0.08 versus 0.30 admissions per block [A/blk], p < 0.001), as than 2003-PIIIa. Similarly in 2010-PIIIb and PVb, where one block of cytarabine was replaced by two doses of vincristine, admissions for fever were also fewer (0.47 versus 0.74 A/blk, p < 0.001) than in 2003-PIIIb. However, the addition of single doses of vincristine and asparaginase in 2010-PIIIa, even with a mandatory seven-day rest, led to more hospitalisations (0.45 A/blk, p < 0.001), increased risk of bacteraemia (relative-risk (RR) = 7.66, p = 0.005) and critical-care admissions (RR = 4.31, p = 0.13). Despite this, overall treatment-related mortality decreased from 2.7% to 0.8%. Taken together, the reduced phase delays allowed earlier completion of the intensive phase of treatment (standard risk: 38.1 versus 49.4 weeks, p < 0.001; intermediate risk: 50.9 versus 58.8 weeks, p < 0.001), while maintaining excellent 10-year event-free survival of 95.4% and overall survival of 96.2%.
CONCLUSIONS
In non-HR ALL, replacing doxorubicin/cytarabine with vincristine/asparaginase during some DI blocks is effective in reducing toxicity without compromising outcomes.
CLINICAL TRIAL INFORMATION
NCT0289464.
背景
在非高危(非 HR)患者中,马来西亚-新加坡急性淋巴细胞白血病 2003 年(MS2003)研究取得了良好的结果。然而,其延迟强化(DI)阶段,包括重复使用方案 III(2003-PIII),具有毒性,并导致显著的治疗延迟。后续的 MS2010 研究试图通过用长春新碱和门冬酰胺酶替代骨髓抑制药物(阿霉素、阿糖胞苷)来降低 DI 毒性。
方法
我们分析了 315 名新加坡非高危急性淋巴细胞白血病(ALL)患儿(MS2003,n=183;MS2010,n=132)的 315 例发热住院病例,占总队列(n=413)的 76%,以研究这些变化的影响。
结果
新的 2010-PVa 不含阿霉素,与 2003-PIIIa 相比,因发热而住院的次数明显减少(每块[blk]0.08 次与 0.30 次,p<0.001)。同样,在 2010-PIIIb 和 PVb 中,用两剂长春新碱代替阿糖胞苷一个blk 时,发热住院也减少(0.47 次与 0.74 次,p<0.001)。然而,在 2010-PIIIa 中添加单次剂量的长春新碱和门冬酰胺酶,即使有七天的强制性休息,也会导致更多的住院(0.45 次/blk,p<0.001),增加菌血症的风险(相对风险[RR]为 7.66,p=0.005)和重症监护病房入院(RR 为 4.31,p=0.13)。尽管如此,总的治疗相关死亡率从 2.7%下降到 0.8%。总的来说,减少阶段延迟使得密集治疗阶段更早完成(标准风险:38.1 周与 49.4 周,p<0.001;中间风险:50.9 周与 58.8 周,p<0.001),同时保持了 10 年无事件生存率 95.4%和总生存率 96.2%的优异水平。
结论
在非高危 ALL 中,在某些 DI 块中用长春新碱/门冬酰胺酶代替阿霉素/阿糖胞苷可有效降低毒性,而不影响结果。
临床试验信息
NCT0289464。
Zotero 插件