| Literature DB >> 25465126 |
Tri Nguyen1, Elisa Hawkins1, Akhil Kolluri1, Maciej Kmieciak2, Haeseong Park1, Hui Lin1, Steven Grant3.
Abstract
Interactions between the dual BCR/ABL and Src inhibitor bosutinib and the Chk1 inhibitor PF-00477736 were examined in BCR/ABL(+) leukemia cells, particularly imatinib-resistant cells, including those with the T315I mutation. Bosutinib blocked PF-00477736-induced ERK1/2 activation and sharply increased apoptosis in association with Mcl-1 inhibition, p34(cdc2) dephosphorylation, BimEL up-regulation, and DNA damage in imatinib-resistant CML or Ph(+) ALL cell lines. Inhibition of Src or MEK1 by shRNA significantly enhanced PF-0047736 lethality. Bosutinib/PF-00477736 co-treatment also potentiated cell death in CD34(+) CML patient samples, including dasatinib-resistant blast crisis cells exhibiting both T315I and E355G mutations, but was minimally toxic to normal CD34(+) cells. Finally, combined in vivo treatment significantly suppressed BaF3/T315I tumor growth and prolonged survival in an allogeneic mouse model. Together, these findings suggest that this targeted combination strategy warrants attention in IM-resistant CML or Ph(+) ALL.Entities:
Keywords: BCR/ABL; Bosutinib; Chk1 inhibitor; Chronic myeloid leukemia
Mesh:
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Year: 2014 PMID: 25465126 PMCID: PMC4413916 DOI: 10.1016/j.leukres.2014.10.009
Source DB: PubMed Journal: Leuk Res ISSN: 0145-2126 Impact factor: 3.156