Authors
Richard C Harvey, Charles G Mullighan, Xuefei Wang, Kevin K Dobbin, George S Davidson, Edward J Bedrick, I-Ming Chen, Susan R Atlas, Huining Kang, Kerem Ar, Carla S Wilson, Walker Wharton, Maurice Murphy, Meenakshi Devidas, Andrew J Carroll, Michael J Borowitz, W Paul Bowman, James R Downing, Mary Relling, Jun Yang, Deepa Bhojwani, William L Carroll, Bruce Camitta, Gregory H Reaman, Malcolm Smith, Stephen P Hunger, Cheryl L Willman
Publication date
2010/12/2
Journal
Blood, The Journal of the American Society of Hematology
Volume
116
Issue
23
Pages
4874-4884
Publisher
American Society of Hematology
Description
To resolve the genetic heterogeneity within pediatric high-risk B-precursor acute lymphoblastic leukemia (ALL), a clinically defined poor-risk group with few known recurring cytogenetic abnormalities, we performed gene expression profiling in a cohort of 207 uniformly treated children with high-risk ALL. Expression profiles were correlated with genome-wide DNA copy number abnormalities and clinical and outcome features. Unsupervised clustering of gene expression profiling data revealed 8 unique cluster groups within these high-risk ALL patients, 2 of which were associated with known chromosomal translocations (t(1;19)(TCF3-PBX1) or MLL), and 6 of which lacked any previously known cytogenetic lesion. One unique cluster was characterized by high expression of distinct outlier genes AGAP1, CCNJ, CHST2/7, CLEC12A/B, and PTPRM; ERG DNA deletions; and 4-year relapse-free survival of 94.7% ± 5 …
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Scholar articles
RC Harvey, CG Mullighan, X Wang, KK Dobbin… - Blood, The Journal of the American Society of …, 2010