Search for Synergistic Drug Combinations to Treat Chronic Lymphocytic Leukemia

Eleonora Ela Hezkiy; Santosh Kumar; Valid Gahramanov; Julia Yaglom; Arkadi Hesin; Suchita Suryakant Jadhav; Ekaterina Guzev; Shivani Patel; Elena Avinery; Michael A. Firer; Michael Y. Sherman

doi:10.3390/cells11223671

Cells (Nov 2022)

Search for Synergistic Drug Combinations to Treat Chronic Lymphocytic Leukemia

Eleonora Ela Hezkiy,
Santosh Kumar,
Valid Gahramanov,
Julia Yaglom,
Arkadi Hesin,
Suchita Suryakant Jadhav,
Ekaterina Guzev,
Shivani Patel,
Elena Avinery,
Michael A. Firer,
Michael Y. Sherman

Affiliations

Eleonora Ela Hezkiy: Department of Molecular Biology, Ariel University, Ariel 40700, Israel
Santosh Kumar: Department of Molecular Biology, Ariel University, Ariel 40700, Israel
Valid Gahramanov: Department of Molecular Biology, Ariel University, Ariel 40700, Israel
Julia Yaglom: Department of Molecular Biology, Ariel University, Ariel 40700, Israel
Arkadi Hesin: Department of Molecular Biology, Ariel University, Ariel 40700, Israel
Suchita Suryakant Jadhav: Department of Chemical Engineering, Ariel University, Ariel 40700, Israel
Ekaterina Guzev: Department of Mathematics, Ariel University, Ariel 40700, Israel
Shivani Patel: Department of Molecular Biology, Ariel University, Ariel 40700, Israel
Elena Avinery: Department of Molecular Biology, Ariel University, Ariel 40700, Israel
Michael A. Firer: Department of Chemical Engineering, Ariel University, Ariel 40700, Israel
Michael Y. Sherman: Department of Molecular Biology, Ariel University, Ariel 40700, Israel

DOI: https://doi.org/10.3390/cells11223671
Journal volume & issue: Vol. 11, no. 22
p. 3671

Abstract

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Finding synergistic drug combinations is an important area of cancer research. Here, we sought to rationally design synergistic drug combinations with an inhibitor of BTK kinase, ibrutinib, which is used for the treatment of several types of leukemia. We (a) used a pooled shRNA screen to identify genes that protect cells from the drug, (b) identified protective pathways via bioinformatics analysis of these gene sets, and (c) identified drugs that inhibit these pathways. Based on this analysis, we established that inhibitors of proteasome and mTORC1 could synergize with ibrutinib both in vitro and in vivo. We suggest that FDA-approved inhibitors of these pathways could be effectively combined with ibrutinib for the treatment of chronic lymphocytic leukemia (CLL).

Published in Cells

ISSN: 2073-4409 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Science: Biology (General): Cytology
Website: https://www.mdpi.com/journal/cells

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