DNA damage–induced transcriptional program in CLL: biological and diagnostic implications for functional p53 testing

Author:

Mohr Julia1,Helfrich Hanne1,Fuge Maxi1,Eldering Eric2,Bühler Andreas1,Winkler Dirk1,Volden Matthias1,Kater Arnon P.3,Mertens Daniel1,Te Raa Doreen3,Döhner Hartmut1,Stilgenbauer Stephan1,Zenz Thorsten1

Affiliation:

1. Department of Internal Medicine III, University of Ulm, Ulm, Germany; and

2. Laboratory of Experimental Immunology and

3. Department of Hematology, Academic Medical Centre, Amsterdam, The Netherlands

Abstract

Abstract The DNA damage pathway plays a central role in chemoresistance in chronic lymphocytic leukemia (CLL), as indicated by the prognostic impact of TP53 and ATM loss/mutations. We investigated the function of the p53 axis in primary CLL samples by studying p53 and p21 responses to irradiation by FACS and RT-PCR. We observed a distinct response pattern for most cases with a 17p deletion (n = 16) or a sole TP53 mutation (n = 8), but not all cases with a p53 aberration were detected based on a number of different assays used. Samples with a small clone with a TP53 mutation remained undetected in all assays. Only 1 of 123 cases showed high expression of p53, which is suggestive of p53 aberration without proof of mutation of TP53. Samples with an 11q deletion showed a heterogeneous response, with only 13 of 30 showing an abnormal response based on cutoff. Nevertheless, the overall induction of p53 and p21 was impaired, suggesting a gene-dosage effect for ATM in the 11q-deleted samples. The detectability of p53 defects is influenced by clonal heterogeneity and sample purity. Functional assays of p53 defects will detect a small number of cases not detectable by FISH or TP53 mutational analysis. The clinical utility of functional p53 testing will need to be derived from clinical trials.

Publisher

American Society of Hematology

Subject

Cell Biology,Hematology,Immunology,Biochemistry

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