Resistance to the BCL-XL degrader DT2216 in T-cell acute lymphoblastic leukemia is rare and correlates with decreased BCL-XL proteolysis.

Arunima JaiswalAruna JaiswalElizabeth A WilliamsonJonathon GelfondGuangrong ZhengDaohong ZhouRobert Hromas

Published in: Cancer chemotherapy and pharmacology (2022)

Resistance to DT2216 is rare in a wide variety of T-ALL cells but when it occurs is correlated with decreased BCL-XL degradation. Resistance to DT2216 in T-ALL is not predicted by initial BCL-XL or BIM protein levels, or BCL-2 or MCL-1 levels before or after treatment. These data imply that a phase 2 clinical trial of DT2216 in T-ALL should be widely available and not limited to a subset of patients.

Keyphrases

acute lymphoblastic leukemia
clinical trial
end stage renal disease
ejection fraction
induced apoptosis
newly diagnosed
chronic kidney disease
prognostic factors
randomized controlled trial
machine learning
cell cycle arrest
big data
study protocol
acute myeloid leukemia
signaling pathway