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Therapeutic implications of Src independent calcium mobilization in diffuse large B-cell lymphoma

Date Issued
2010-01-01
Author(s)
Hollmann, C Annette
Tzankov, Alexandar  
Martínez-Marignac, Verónica L
Baker, Kristi
Grygorczyk, Czeslawa
Grygorczyk, Ryszard
Foulkes, William
Nadeau, Jay
Dirnhofer, Stephan  
Aloyz, Raquel
DOI
10.1016/j.leukres.2009.08.030
Abstract
We report that 38% of primary large B-cell lymphoma (DLBCL) tested expressed active Src family kinases, which are targeted by dasatinib. The expression of active Src family of kinases (SFK) in primary DLBCL tumors correlated with unfavorable prognostic markers such as Ki67 and Mum1. Using four DLBCL cell lines we found that: (1) sensitivity to dasatinib (but not imatinib) varied 400-fold; (2) dasatinib resistance was associated with distinct signaling profiles downstream of BCR activation. In particular, although Src family kinase phosphorylation was inhibited by 100-150 nM dasatinib in all cell lines, this failed to inhibit BCR-mediated Blnk phosphorylation, calcium signaling and proliferation in a dasatinib resistant cell line.
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