Transcriptomic classes of BCR-ABL1 lymphoblastic leukemia

被引:0
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作者
Jaeseung C. Kim
Michelle Chan-Seng-Yue
Sabrina Ge
Andy G. X. Zeng
Karen Ng
Olga I. Gan
Laura Garcia-Prat
Eugenia Flores-Figueroa
Tristan Woo
Amy Xin Wei Zhang
Andrea Arruda
Shivapriya Chithambaram
Stephanie M. Dobson
Amanda Khoo
Shahbaz Khan
Narmin Ibrahimova
Ann George
Anne Tierens
Johann Hitzler
Thomas Kislinger
John E. Dick
John D. McPherson
Mark D. Minden
Faiyaz Notta
机构
[1] Princess Margaret Cancer Centre,Department of Medical Biophysics
[2] Ontario Institute for Cancer Research,undefined
[3] University of Toronto,undefined
[4] The Hospital for Sick Children,undefined
[5] University of California Davis Comprehensive Cancer Center,undefined
来源
Nature Genetics | 2023年 / 55卷
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摘要
In BCR-ABL1 lymphoblastic leukemia, treatment heterogeneity to tyrosine kinase inhibitors (TKIs), especially in the absence of kinase domain mutations in BCR-ABL1, is poorly understood. Through deep molecular profiling, we uncovered three transcriptomic subtypes of BCR-ABL1 lymphoblastic leukemia, each representing a maturation arrest at a stage of B-cell progenitor differentiation. An earlier arrest was associated with lineage promiscuity, treatment refractoriness and poor patient outcomes. A later arrest was associated with lineage fidelity, durable leukemia remissions and improved patient outcomes. Each maturation arrest was marked by specific genomic events that control different transition points in B-cell development. Interestingly, these events were absent in BCR-ABL1+ preleukemic stem cells isolated from patients regardless of subtype, which supports that transcriptomic phenotypes are determined downstream of the leukemia-initialing event. Overall, our data indicate that treatment response and TKI efficacy are unexpected outcomes of the differentiation stage at which this leukemia transforms.
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页码:1186 / 1197
页数:11
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