| Literature DB >> 19587702 |
J Familiades1, M Bousquet, M Lafage-Pochitaloff, M-C Béné, K Beldjord, J De Vos, N Dastugue, E Coyaud, S Struski, C Quelen, N Prade-Houdellier, S Dobbelstein, J-M Cayuela, J Soulier, N Grardel, C Preudhomme, H Cavé, O Blanchet, V Lhéritier, A Delannoy, Y Chalandon, N Ifrah, A Pigneux, P Brousset, E A Macintyre, F Huguet, H Dombret, C Broccardo, E Delabesse.
Abstract
Adult and child B-cell progenitor acute lymphoblastic leukemia (BCP-ALL) differ in terms of incidence and prognosis. These disparities are mainly due to the molecular abnormalities associated with these two clinical entities. A genome-wide analysis using oligo SNP arrays recently demonstrated that PAX5 (paired-box domain 5) is the main target of somatic mutations in childhood BCP-ALL being altered in 38.9% of the cases. We report here the most extensive analysis of alterations of PAX5 coding sequence in 117 adult BCP-ALL patients in the unique clinical protocol GRAALL-2003/GRAAPH-2003. Our study demonstrates that PAX5 is mutated in 34% of adult BCP-ALL, mutations being partial or complete deletion, partial or complete amplification, point mutation or fusion gene. PAX5 alterations are heterogeneous consisting in complete loss in 17%, focal deletions in 10%, point mutations in 7% and translocations in 1% of the cases. PAX5 complete loss and PAX5 point mutations differ. PAX5 complete loss seems to be a secondary event and is significantly associated with BCR-ABL1 or TCF3-PBX1 fusion genes and a lower white blood cell count.Entities:
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Year: 2009 PMID: 19587702 DOI: 10.1038/leu.2009.135
Source DB: PubMed Journal: Leukemia ISSN: 0887-6924 Impact factor: 11.528