Prediction of venetoclax activity in precursor B-ALL by functional assessment of apoptosis signaling.
Felix SeyfriedSalih DemirRebecca Louise HörlFelix Uli StirnweißJeremy Adam RyanAnnika ScheffoldMariana Villalobos-OrtizElena BoldrinJulia ZinngrebeStefanie EnzenmüllerSilvia JenniYi-Chien TsaiBeat BornhauserAxel FürstbergerJohann Michael KrausHans Armin KestlerJean-Pierre BourquinStephan StilgenbauerAnthony LetaiKlaus-Michael DebatinLüder Hinrich MeyerPublished in: Cell death & disease (2019)
Deregulated cell death pathways contribute to leukemogenesis and treatment failure in B-cell precursor acute lymphoblastic leukemia (BCP-ALL). Intrinsic apoptosis signaling is regulated by different proapoptotic and antiapoptotic molecules: proapoptotic BCL-2 homology domain 3 (BH3) proteins activate prodeath molecules leading to cellular death, while antiapoptotic molecules including B-cell lymphoma 2 (BCL-2) prevent activation of prodeath proteins and counter-regulate apoptosis induction. Inhibition of these antiapoptotic regulators has become a promising strategy for anticancer treatment, but variable anticancer activities in different malignancies indicate the need for upfront identification of responsive patients. Here, we investigated the activity of the BCL-2 inhibitor venetoclax (VEN, ABT-199) in B-cell precursor acute lymphoblastic leukemia and found heterogeneous sensitivities in BCP-ALL cell lines and in a series of patient-derived primografts. To identify parameters of sensitivity and resistance, we evaluated genetic aberrations, gene-expression profiles, expression levels of apoptosis regulators, and functional apoptosis parameters analyzed by mitochondrial profiling using recombinant BH3-like peptides. Importantly, ex vivo VEN sensitivity was most accurately associated with functional BCL-2 dependence detected by BH3 profiling. Modeling clinical application of VEN in a preclinical trial in a set of individual ALL primografts, we identified that leukemia-free survival of VEN treated mice was precisely determined by functional BCL-2 dependence. Moreover, the predictive value of ex vivo measured functional BCL-2 dependence for preclinical in vivo VEN response was confirmed in an independent set of primograft ALL including T- and high risk-ALL. Thus, integrative analysis of the apoptosis signaling indicating mitochondrial addiction to BCL-2 accurately predicts antileukemia activity of VEN, robustly identifies VEN-responsive patients, and provides information for stratification and clinical guidance in future clinical applications of VEN in patients with ALL.
Keyphrases
- cell death
- oxidative stress
- cell cycle arrest
- acute lymphoblastic leukemia
- endoplasmic reticulum stress
- end stage renal disease
- newly diagnosed
- ejection fraction
- free survival
- genome wide
- chronic kidney disease
- transcription factor
- stem cells
- pi k akt
- randomized controlled trial
- bone marrow
- clinical trial
- single cell
- poor prognosis
- signaling pathway
- mesenchymal stem cells
- combination therapy
- long non coding rna
- current status
- mass spectrometry
- social media
- insulin resistance
- high resolution
- network analysis
- health information
- study protocol
- genome wide analysis