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Clinical impact of minimal residual disease and genetic subtypes on the prognosis of childhood acute lymphoblastic leukemia

医学 微小残留病 达沙替尼 队列 肿瘤科 诱导化疗 白血病 内科学 免疫学 化疗 伊马替尼 髓系白血病
作者
Chih‐Hsiang Yu,Shiann‐Tarng Jou,Ying‐Hui Su,Elane Coustan‐Smith,Gang Wu,Chao‐Neng Cheng,Meng‐Yao Lu,Kai‐Hsin Lin,Kang‐Hsi Wu,Shu‐Huey Chen,Fang‐Liang Huang,Hong‐Yeh Chang,Jinn‐Li Wang,Hsiu‐Ju Yen,Meng‐Ju Li,Shu‐Wei Chou,Wan‐Ling Ho,Yen‐Lin Liu,Chia‐Hao Chang,Ze‐Shiang Lin,Chien‐Yu Lin,Hsuan‐Yu Chen,Yu‐Ling Ni,Dong‐Tsamn Lin,Shu‐Wha Lin,Jun J. Yang,Yen‐Hsuan Ni,Ching‐Hon Pui,Sung‐Liang Yu,Yung‐Li Yang
出处
期刊:Cancer [Wiley]
卷期号:129 (5): 790-802 被引量:1
标识
DOI:10.1002/cncr.34606
摘要

This study analyzed data from two consecutive protocols for children newly diagnosed with acute lymphoblastic leukemia (ALL) to determine the clinical impact of minimal/measurable residual disease (MRD) and recently identified tumor genetic subtypes.Genetic subtypes were determined by sequential approaches including DNA indexing, reverse transcriptase-polymerase chain reaction, multiplex ligation-dependent probe amplification, and RNA-sequencing. MRD was assessed by flow cytometry. The Taiwan Pediatric Oncology Group TPOG-ALL-2013 study enrolled patients who received MRD-directed therapy.The 5-year event-free survival (EFS) and overall survival rates in the 2013 cohort were 77.8% and 86.9% compared to those of the 2002 cohort, which were 62.4% and 76.5%. Among patients treated with MRD-guided therapy, those with ETV6-RUNX1 fusion and high hyperdiploidy had the highest 5-year EFS (91.4% and 89.6%, respectively). The addition of dasatinib improved outcomes in patients with BCR-ABL1 ALL. Recently identified subtypes like DUX4-rearranged, ZNF384-rearranged, MEF2D-rearranged, and PAX5alt subtypes were frequently positive for MRD after remission induction, and these patients consequently received intensified chemotherapy. Treatment intensification according to the MRD improved the outcomes of patients presenting DUX4 rearrangements. In high-risk or very-high-risk subtypes, the TPOG-ALL-2013 regimen did not confer significant improvements compared to TPOG-ALL-2002, and the outcomes of BCR-ABL1-like, MEF2D-rearranged, and KMT2A-rearranged ALL subtypes (in addition to those of T-cell ALL) were not sufficiently good. Novel agents or approaches are needed to improve the outcomes for these patients.The TPOG-ALL-2013 study yielded outcomes superior to those of patients treated in the preceding TPOG-ALL-2002 study. This study provides important data to inform the design of future clinical trials in Taiwan.MRD-directed therapy improved the outcomes for pediatric ALL, especially standard-risk patients. Genomic analyses and MRD might be used together for risk-directed therapy of childhood ALL. Our work provides important data to inform the design of future clinical trials in Taiwan.

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