INSERM Clinical Investigation Center 1402, Poitiers University, Poitiers, France.
Department of Pediatrics, Carl Gustav Carus University Hospital, Dresden, Germany.
Cancer. 2017 Sep 15;123(18):3609-3616. doi: 10.1002/cncr.30767. Epub 2017 May 12.
In the adult population with newly diagnosed chronic myeloid leukemia (CML), variant translocations are usually not considered to be impairing the prognosis, whereas some additional cytogenetic abnormalities (ACAs) are associated with a negative impact on survival. Because of the rarity of CML in the pediatric population, such abnormalities have not been investigated in a large group of children with CML.
The prognostic relevance of variant t(9;22) and ACAs at diagnosis was assessed in 301 children with CML in the chronic phase who were enrolled in the International Registry for Chronic Myeloid Leukemia in Children and Adolescents.
Overall, 19 children (6.3%) presented with additional cytogenetic findings at diagnosis: 5 children (1.7%) had a variant t(9;22) translocation, 13 children (4.3%) had ACAs, and 1 had both. At 3 years, for children with a classic translocation, children with ACAs, and children with a variant t(9;22) translocation who were treated with imatinib as frontline therapy, the probability of progression-free survival (PFS) was 95% (95% confidence interval [CI], 91%-97%), 100%, and 75% (95% CI, 13%-96%), respectively, and the probability of overall survival (OS) was 98% (95% CI, 95%-100%), 100% (95% CI, 43%-98%), and 75% (95% CI, 13%-96%), respectively. No statistical difference was observed between the patients with classic cytogenetic findings and those with additional chromosomal abnormalities in terms of PFS and OS.
In contrast to adults with CML, additional chromosomal abnormalities observed at diagnosis do not seem to have a significant prognostic impact. Cancer 2017;123:3609-16. © 2017 American Cancer Society.
在新诊断为慢性髓性白血病(CML)的成人患者中,变体易位通常不被认为会影响预后,而一些额外的细胞遗传学异常(ACAs)与生存的负面影响有关。由于儿童人群中 CML 较为罕见,因此尚未在大量 CML 患儿中研究此类异常。
在国际儿童和青少年慢性髓性白血病登记处登记的 301 名处于慢性期的 CML 患儿中,评估了诊断时变体 t(9;22)和 ACAs 的预后相关性。
总体而言,19 名患儿(6.3%)在诊断时存在额外的细胞遗传学发现:5 名患儿(1.7%)存在变体 t(9;22)易位,13 名患儿(4.3%)存在 ACAs,1 名患儿同时存在两者。在 3 年时,对于经典易位的患儿、存在 ACAs 的患儿和以伊马替尼作为一线治疗的存在变体 t(9;22)易位的患儿,无进展生存(PFS)的概率分别为 95%(95%置信区间[CI],91%-97%)、100%和 75%(95%CI,13%-96%),总生存(OS)的概率分别为 98%(95%CI,95%-100%)、100%(95%CI,43%-98%)和 75%(95%CI,13%-96%)。在 PFS 和 OS 方面,具有经典细胞遗传学发现的患者与具有额外染色体异常的患者之间未观察到统计学差异。
与 CML 成人患者不同,诊断时观察到的额外染色体异常似乎没有显著的预后影响。癌症 2017;123:3609-16。©2017 美国癌症协会。
