Targeting mutant TP53 in ALL

S Demir; G Selivanova; E Tausch; L Wiesmüller; S Stilgenbauer; G te Kronnie; KM Debatin; LH Meyer

doi:10.1055/s-0036-1582498

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Klin Padiatr 2016; 228 - A21
DOI: 10.1055/s-0036-1582498

Targeting mutant TP53 in ALL

S Demir ¹, G Selivanova ², E Tausch ¹, L Wiesmüller ¹, S Stilgenbauer ¹, G te Kronnie ³, KM Debatin ¹, LH Meyer ¹

¹Ulm University Medical Center, Germany
²Karolinska Institute, Sweden
³Padova University, Padova, Italy

Congress Abstract

Introduction: In ALL, TP53 mutations (TP53mut) are increased at relapse and associated with poor prognosis and resistance. APR-246 binds to mutant p53 and restoring wt conformation.

Methods: TP53mut were analyzed by dHPLC and Sanger sequencing, apoptosis by AnnexinV/PI, p53 targets by western blotting, p53 silencing by lentiviral shRNA, and phosphorylation by phosphoflow cytometry.

Results: APR-246 exposure led to apoptosis in TP53mut ALL and induced functional p53 re-activation indicated by p53Ser15 phosphorylation including expression of downstream targets in a p53 dependent manner in TP53mut but not TP53wt ALL. Additionally, APR-246 re-sensitized TP53mut resistant leukemias strongly synergizing with the DNA-damage inducer doxorubicin.

Conclusion: APR-246 functionally re-activates mutant p53, leading to apoptosis induction and re-sensitization of TP53mut but not TP53wt ALL cells. Thus, targeting mutated p53 provides a promising novel strategy in this high-risk subtype of ALL.