NUP214-ABL1 in adult T-ALL: the GMALL study group experience

T Burmeister, N Gökbuget, R Reinhardt, H Rieder… - Blood, 2006 - ashpublications.org
T Burmeister, N Gökbuget, R Reinhardt, H Rieder, D Hoelzer, S Schwartz
Blood, 2006ashpublications.org
The NUP214-ABL1 fusion gene in T-cell acute lymphoblastic leukemia (T-ALL) has recently
been identified as a possible target for imatinib and related tyrosine kinase inhibitors, but
exact data regarding the prognostic impact and frequency of the several putative NUP214-
ABL1 mRNA transcripts are still missing. We investigated 279 adult patients with T-ALL
treated within the framework of the GMALL 5/93 and 6/99 therapy trials for NUP214-ABL1 by
using a novel multiplex real-time, quantitative polymerase chain reaction (PCR). Eleven …
Abstract
The NUP214-ABL1 fusion gene in T-cell acute lymphoblastic leukemia (T-ALL) has recently been identified as a possible target for imatinib and related tyrosine kinase inhibitors, but exact data regarding the prognostic impact and frequency of the several putative NUP214-ABL1 mRNA transcripts are still missing. We investigated 279 adult patients with T-ALL treated within the framework of the GMALL 5/93 and 6/99 therapy trials for NUP214-ABL1 by using a novel multiplex real-time, quantitative polymerase chain reaction (PCR). Eleven (3.9%) patients were NUP214-ABL1 positive, and 5 different transcripts were observed; 8 patients had a thymic immunophenotype, 1 had an early T-cell immunophenotype, and 2 had a mature T-cell immunophenotype. NUP214-ABL1-positive and -negative patients did not differ significantly in their major clinical features. In contrast to previous reports suggesting an adverse clinical course for NUP214-ABL1-positive patients, no significant difference in overall survival was observed. Based on the results, we have established and tested a novel PCR method for simplified detection of the NUP214-ABL1 fusion gene.
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