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- BCR-ABL down-regulates the DNA repair protein DNA-PKcs
BCR-ABL down-regulates the DNA repair protein DNA-PKcs
Authors
Eric Deutsch, Aymeric Dugray, Bassam AbdulKarim, Elisabetta Marangoni, Laurence Maggiorella, Sabine Vaganay, Radia M'Kacher, Setha Douc Rasy, François Eschwege, William Vainchenker, Ali G. Turhan, Jean Bourhis
Abstract
Abstract
This study demonstrates in both stable and inducible BCR-ABL–expressing hematopoietic cells a down-regulation of the major mammalian DNA repair protein DNA-PKcs by BCR-ABL. Similar results were found in BCR-ABL CD34+ cells from patients with chronic myelogenous leukemia (CML). DNA-PKcs down-regulation is a proteasome-dependent degradation that requires tyrosine kinase activity and is associated with a marked DNA repair deficiency along with increased sensitivity to ionizing radiation. The conjunction of a major DNA repair deficiency and a resistance to apoptosis, both induced by BCR-ABL, provides a new mechanism to explain how secondary genetic alterations can accumulate in CML, eventually leading to blast crisis. The down-regulation of DNA-PKcs was reversible in CD34+ CML cells suggesting that this approach might offer a novel and powerful therapeutic strategy in this disease, especially to delay the blast crisis.