Integrative multi-omics and drug response profiling of childhood acute lymphoblastic leukemia cell lines

Author:

Leo Isabelle RoseORCID,Aswad LuayORCID,Stahl MatthiasORCID,Kunold Elena,Post FrederikORCID,Erkers Tom,Struyf NonaORCID,Mermelekas Georgios,Joshi Rubin Narayan,Gracia-Villacampa EvaORCID,Östling Päivi,Kallioniemi Olli P.,Tamm Katja PokrovskajaORCID,Siavelis Ioannis,Lehtiö JanneORCID,Vesterlund MattiasORCID,Jafari RozbehORCID

Abstract

AbstractAcute lymphoblastic leukemia (ALL) is the most common childhood cancer. Although standard-of-care chemotherapeutics are sufficient for most ALL cases, there are subsets of patients with poor response who relapse in disease. The biology underlying differences between subtypes and their response to therapy has only partially been explained by genetic and transcriptomic profiling. Here, we perform comprehensive multi-omic analyses of 49 readily available childhood ALL cell lines, using proteomics, transcriptomics, and pharmacoproteomic characterization. We connect the molecular phenotypes with drug responses to 528 oncology drugs, identifying drug correlations as well as lineage-dependent correlations. We also identify the diacylglycerol-analog bryostatin-1 as a therapeutic candidate in the MEF2D-HNRNPUL1 fusion high-risk subtype, for which this drug activates pro-apoptotic ERK signaling associated with molecular mediators of pre-B cell negative selection. Our data is the foundation for the interactive online Functional Omics Resource of ALL (FORALL) with navigable proteomics, transcriptomics, and drug sensitivity profiles at https://proteomics.se/forall.

Funder

Barncancerfonden

Vetenskapsrådet

Stiftelsen Felix Mindus Bidrag till Leukemiforskningen

Cancerföreningen i Stockholm

Dr Åke Olssons Stiftelse för Haematologisk Forskning

Magnus Bergvalls Stiftelse

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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