| Literature DB >> 23223358 |
Jamshid S Khorashad1, Todd W Kelley, Philippe Szankasi, Clinton C Mason, Simona Soverini, Lauren T Adrian, Christopher A Eide, Matthew S Zabriskie, Thoralf Lange, Johanna C Estrada, Anthony D Pomicter, Anna M Eiring, Ira L Kraft, David J Anderson, Zhimin Gu, Mary Alikian, Alistair G Reid, Letizia Foroni, David Marin, Brian J Druker, Thomas O'Hare, Michael W Deininger.
Abstract
BCR-ABL1 compound mutations can confer high-level resistance to imatinib and other ABL1 tyrosine kinase inhibitors (TKIs). The third-generation ABL1 TKI ponatinib is effective against BCR-ABL1 point mutants individually, but remains vulnerable to certain BCR-ABL1 compound mutants. To determine the frequency of compound mutations among chronic myeloid leukemia patients on ABL1 TKI therapy, in the present study, we examined a collection of patient samples (N = 47) with clear evidence of 2 BCR-ABL1 kinase domain mutations by direct sequencing. Using a cloning and sequencing method, we found that 70% (33/47) of double mutations detected by direct sequencing were compound mutations. Sequential, branching, and parallel routes to compound mutations were common. In addition, our approach revealed individual and compound mutations not detectable by direct sequencing. The frequency of clones harboring compound mutations with more than 2 missense mutations was low (10%), whereas the likelihood of silent mutations increased disproportionately with the total number of mutations per clone, suggesting a limited tolerance for BCR-ABL1 kinase domain missense mutations. We conclude that compound mutations are common in patients with sequencing evidence for 2 BCR-ABL1 mutations and frequently reflect a highly complex clonal network, the evolution of which may be limited by the negative impact of missense mutations on kinase function.Entities:
Mesh:
Substances:
Year: 2012 PMID: 23223358 PMCID: PMC3548169 DOI: 10.1182/blood-2012-05-431379
Source DB: PubMed Journal: Blood ISSN: 0006-4971 Impact factor: 22.113