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治疗相关白血病和骨髓增生异常综合征:临床、细胞遗传学及预后特征

Therapy-related leukemia and myelodysplastic syndrome: clinical, cytogenetic, and prognostic features.

作者信息

Kantarjian H M, Keating M J, Walters R S, Smith T L, Cork A, McCredie K B, Freireich E J

出版信息

J Clin Oncol. 1986 Dec;4(12):1748-57. doi: 10.1200/JCO.1986.4.12.1748.

DOI:10.1200/JCO.1986.4.12.1748
PMID:3783201
Abstract

One hundred twelve patients who developed acute leukemia or a myelodysplastic syndrome (MDS) after chemotherapy or irradiation for another malignancy were reviewed. The median time from initial therapy to development of secondary leukemia or MDS was 71 months (range, 7 to 331 months). The initial malignancy was hematologic in 43%. An MDS presentation occurred in 57 patients (51%), 55% of whom subsequently transformed to acute leukemia. Chromosomal abnormalities were documented in marrow specimens from 70 of 89 patients with analyzable metaphases (79%; 69% of the total group). Compared with 34 patients with metachronous secondary leukemia without prior chemotherapy or irradiation, those with therapy-related leukemia exhibited a significantly higher frequency of abnormalities of chromosomes 5 and/or 7 (43% v 18%), and lower incidence of diploid karyotypes (18% v 50%). Chromosome 5 and/or 7 abnormalities were also significantly higher in patients previously treated with alkylating agents, procarbazine, and nitrosoureas (72% to 83%), compared with those who had received cyclophosphamide-based regimens (29%), other chemotherapies (14%), or irradiation alone (29%). The median overall survival from diagnosis of the secondary leukemia or MDS was 30 weeks. Survival was significantly shorter for patients with acute leukemia compared with MDS presentation (21 v 45 weeks); in the latter category, it was similar whether evolution to acute leukemia occurred or not. Of 72 patients treated with antileukemia therapy, 29% achieved complete remission (CR). A multivariate analysis of prognostic factors demonstrated the cytogenetic pattern to be the most important characteristic determining remission rate and survival. Other important prognostic features were the morphologic presentation (MDS v acute leukemia) for probability of achieving remission, and patient age and marrow blasts percentage for survival.

摘要

对112例在因其他恶性肿瘤接受化疗或放疗后发生急性白血病或骨髓增生异常综合征(MDS)的患者进行了回顾性研究。从初始治疗到继发白血病或MDS发生的中位时间为71个月(范围7至331个月)。43%的患者初始恶性肿瘤为血液系统疾病。57例患者(51%)表现为MDS,其中55%随后转变为急性白血病。89例有可分析中期分裂相的患者中,70例(79%;占总患者组的69%)骨髓标本记录到染色体异常。与34例无先前化疗或放疗的异时性继发白血病患者相比,治疗相关白血病患者染色体5和/或7异常的频率显著更高(43%对18%),二倍体核型的发生率更低(18%对50%)。与接受环磷酰胺方案(29%)、其他化疗(14%)或单纯放疗(29%)的患者相比,先前接受烷化剂、丙卡巴肼和亚硝基脲治疗的患者染色体5和/或7异常也显著更高(72%至83%)。继发白血病或MDS诊断后的中位总生存期为30周。急性白血病患者的生存期明显短于MDS表现的患者(21周对45周);在MDS患者中,无论是否演变为急性白血病,生存期相似。72例接受抗白血病治疗的患者中,29%达到完全缓解(CR)。预后因素的多变量分析表明,细胞遗传学模式是决定缓解率和生存期的最重要特征。其他重要的预后特征包括达到缓解概率的形态学表现(MDS对急性白血病),以及生存期的患者年龄和骨髓原始细胞百分比。

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