ERK2, but Not ERK1, Mediates Acquired and “De novo” Resistance to Imatinib Mesylate: Implication for CML Therapy |
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Authors: | Clara I Aceves-Luquero Anupriya Agarwal Juan L Callejas-Valera Laura Arias-González Azucena Esparís-Ogando Luis del Peso Ovalle Itxaso Bellón-Echeverria Miguel A de la Cruz-Morcillo Eva M Galán Moya Inmaculada Moreno Gimeno Juan C Gómez Michael W Deininger Atanasio Pandiella Ricardo Sánchez Prieto |
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Institution: | 1. CRIB/Facultad de Medicina, UCLM, Albacete, Spain.; 2. Division of Hematology and Medical Oncology, Oregon Health and Science University Cancer Institute, Portland, Oregon, United States of America.; 3. Instituto de Biología Molecular y Celular del Cáncer, CSIC-USAL, Salamanca, Spain.; 4. Departamento de Bioquímica, Facultad de Medicina, Universidad Autónoma de Madrid, Madrid, Spain.;Roswell Park Cancer Institute, United States of America |
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Abstract: | Resistance to Imatinib Mesylate (IM) is a major problem in Chronic Myelogenous Leukaemia management. Most of the studies about resistance have focused on point mutations on BCR/ABL. However, other types of resistance that do not imply mutations in BCR/ABL have been also described. In the present report we aim to study the role of several MAPK in IM resistance not associate to BCR/ABL mutations. Therefore we used an experimental system of resistant cell lines generated by co-culturing with IM (K562, Lama 84) as well as primary material from resistant and responder patient without BCR/ABL mutations. Here we demonstrate that Erk5 and p38MAPK signaling pathways are not implicated in the acquired resistance phenotype. However, Erk2, but not Erk1, is critical for the acquired resistance to IM. In fact, Bcr/Abl activates preferentially Erk2 in transient transfection in a dose dependent fashion through the c-Abl part of the chimeric protein. Finally, we present evidences demonstrating how constitutive activation of Erk2 is a de novo mechanism of resistance to IM. In summary our data support the use of therapeutic approaches based on Erk2 inhibition, which could be added to the therapeutic armamentarium to fight CML, especially when IM resistance develops secondary to Erk2 activation. |
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