Ex vivo discovery of synergistic drug combinations for hematologic malignancies

Kamran A. Ali; Reecha D. Shah; Anukriti Dhar; Nina M. Myers; Cameron Nguyen; Arisa Paul; Jordan E. Mancuso; A. Scott Patterson; James P. Brody; Diane Heiser

SLAS Discovery (Mar 2024)

Ex vivo discovery of synergistic drug combinations for hematologic malignancies

Kamran A. Ali,
Reecha D. Shah,
Anukriti Dhar,
Nina M. Myers,
Cameron Nguyen,
Arisa Paul,
Jordan E. Mancuso,
A. Scott Patterson,
James P. Brody,
Diane Heiser

Affiliations

Kamran A. Ali: Notable Labs, 320 Hatch Dr, Foster City, CA, 94404, USA; Department of Biomedical Engineering, University of California, Irvine, 3120 Natural Sciences II, Irvine, CA, 92697, USA; Corresponding author.
Reecha D. Shah: Notable Labs, 320 Hatch Dr, Foster City, CA, 94404, USA
Anukriti Dhar: Notable Labs, 320 Hatch Dr, Foster City, CA, 94404, USA
Nina M. Myers: Notable Labs, 320 Hatch Dr, Foster City, CA, 94404, USA
Cameron Nguyen: Notable Labs, 320 Hatch Dr, Foster City, CA, 94404, USA
Arisa Paul: Notable Labs, 320 Hatch Dr, Foster City, CA, 94404, USA
Jordan E. Mancuso: Notable Labs, 320 Hatch Dr, Foster City, CA, 94404, USA
A. Scott Patterson: Notable Labs, 320 Hatch Dr, Foster City, CA, 94404, USA
James P. Brody: Department of Biomedical Engineering, University of California, Irvine, 3120 Natural Sciences II, Irvine, CA, 92697, USA
Diane Heiser: Notable Labs, 320 Hatch Dr, Foster City, CA, 94404, USA

Journal volume & issue: Vol. 29, no. 2
p. 100129

Abstract

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Combination therapies have improved outcomes for patients with acute myeloid leukemia (AML). However, these patients still have poor overall survival. Although many combination therapies are identified with high-throughput screening (HTS), these approaches are constrained to disease models that can be grown in large volumes (e.g., immortalized cell lines), which have limited translational utility. To identify more effective and personalized treatments, we need better strategies for screening and exploring potential combination therapies. Our objective was to develop an HTS platform for identifying effective combination therapies with highly translatable ex vivo disease models that use size-limited, primary samples from patients with leukemia (AML and myelodysplastic syndrome). We developed a system, ComboFlow, that comprises three main components: MiniFlow, ComboPooler, and AutoGater. MiniFlow conducts ex vivo drug screening with a miniaturized flow-cytometry assay that uses minimal amounts of patient sample to maximize throughput. ComboPooler incorporates computational methods to design efficient screens of pooled drug combinations. AutoGater is an automated gating classifier for flow cytometry that uses machine learning to rapidly analyze the large datasets generated by the assay. We used ComboFlow to efficiently screen more than 3000 drug combinations across 20 patient samples using only 6 million cells per patient sample. In this screen, ComboFlow identified the known synergistic combination of bortezomib and panobinostat. ComboFlow also identified a novel drug combination, dactinomycin and fludarabine, that synergistically killed leukemic cells in 35 % of AML samples. This combination also had limited effects in normal, hematopoietic progenitors. In conclusion, ComboFlow enables exploration of massive landscapes of drug combinations that were previously inaccessible in ex vivo models. We envision that ComboFlow can be used to discover more effective and personalized combination therapies for cancers amenable to ex vivo models.

Published in SLAS Discovery

ISSN: 2472-5552 (Print); 2472-5560 (Online)
Publisher: Elsevier
Country of publisher: United States
LCC subjects: Medicine: Medicine (General); Technology: Chemical technology: Biotechnology
Website: https://www.journals.elsevier.com/slas-discovery

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