TEL gene rearrangement in acute lymphoblastic leukemia: A new genetic marker with prognostic significance

Purpose: TEL gene rearrangements due to the 12;21 chromosomal translocation are the most common molecular genetic abnormality in childhood acute lymphoblastic leukemia (ALL), occurring in approximately 25% of cases with a B-precursor immunophenotype. The limited number of clinically useful genetic markers in this leukemia subtype prompted vs to assess TEL status as a predictor of treatment outcome. Patients and Methods: We determined the status of the TEL gene (rearranged or germline) in 188 cases of B-precursor acute leukemia using Southern blot analysis and related the findings to event-free survival. All comparisons of outcome were stratified by treatment regimen, risk classification, age, and leukocyte count. Results: Forty-eight patients (26%) had a rearranged TEL gene, At 5 years of follow-up, an estimated 91% +/- 5% (SE) of this group were event-free survivors, compared with only 65% +/- 5% of the group with germline TEL (stratified log-rank P = .011), For nonhyperdiploid patients, the odds ratio of an adverse event in the germline TEL group to that for the rearranged TEL group was 4.06 (95% confidence interval, 1.86 to 8.84), The relationship of TEL rearrangement to a favorable prognosis was independent of recognised good-risk features in B-precursor leukemia, including age, initial leukocyte count,and hyperdiploidy. Conclusion: Rearrangement of the TEL gene distinguishes a large subset of children with favorable-prognosis B-precursor leukemia who cannot be identified by standard prognostic features. It may be possible to treat these patients less aggressively without loss of therapeutic efficacy. (C) 1997 by American Society of Clinical Oncology.