Journal
GENES CHROMOSOMES & CANCER
Volume 56, Issue 4, Pages 303-313Publisher
WILEY
DOI: 10.1002/gcc.22438
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Funding
- MEXT [25134721, 25830141, 26640110]
- AMED [14524362]
- CREST
- JST
- Foundation for Promotion of Cancer Research
- Kato Memorial Bioscience Foundation [14531766]
- Novartis Pharma KK (Tokyo, Japan)
- Grants-in-Aid for Scientific Research [16H05419, 26640110, 25830141] Funding Source: KAKEN
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Gastrointestinal stromal tumors represent the most common mesenchymal tumor of the digestive tract, driven by gain-of-function mutations in KIT. Despite its proven benefits, half of the patients treated with imatinib show disease progression within 2years due to secondary resistance mutations in KIT. It remains unclear how the genomic and transcriptomic features change during the acquisition of imatinib resistance. Here, we performed exome sequencing and microarray transcription analysis for four imatinib-resistant cell lines and one cell line briefly exposed to imatinib. We also performed exome sequencing of clinical tumor samples. The cell line briefly exposed to imatinib exhibited few single-nucleotide variants and copy-number alterations, but showed marked upregulation of genes related to detoxification and downregulation of genes involved in cell cycle progression. Meanwhile, resistant cell lines harbored numerous genomic changes: amplified genes related to detoxification and deleted genes with cyclin-dependent kinase activity. Some variants in the resistant samples were traced back to the drug-sensitive samples, indicating the presence of ancestral subpopulations. The subpopulations carried variants associated with cell death. Pre-existing cancer cells with genetic alterations promoting apoptosis resistance may serve as a basis whereby cancer cells with critical mutations, such as secondary KIT mutations, can establish full imatinib resistance. (C) 2017 The Authors Genes, Chromosomes and Cancer Published by Wiley Periodicals, Inc.
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