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Combination screen in multi-cell type tumor spheroids reveals interaction between aryl hydrocarbon receptor antagonists and E1 ubiquitin-activating enzyme inhibitor: Aryl-hydrocarbon receptor antagonist drug combinations

  1. Author:
    Dexheimer,Tom
    Coussens,Nathan
    Silvers,Thomas
    Jones,Eric
    Chen,Lily
    Fang, Jianwen
    Morris, Joel
    Moscow, Jeffrey A
    Doroshow, James H
    Teicher, Beverly A

  2. Author Address

    Target Validation and Screening Laboratory, Applied and Developmental Research Directorate. Electronic address: thomas.dexheimer@nih.gov., Molecular Characterization Laboratory, Clinical Research Directorate, Frederick National Laboratory for Cancer Research, Frederick, Maryland, 21702., Division of Cancer Treatment and Diagnosis, National Cancer Institute, National Institutes of Health, Bethesda, Maryland, 20892.,
    1. Year: 2024
    2. Date: Oct 01
    3. Epub Date: 2024 10 01
  2. Journal: SLAS Discovery : advancing life sciences R & D
    1. 29
    2. 7
    3. Pages: 100186
  4. Type of Article: Article
  5. Article Number: 100186
  1. Abstract:

    The aryl hydrocarbon receptor (AhR) is a ligand-activated transcription factor that regulates genes of drug transporters and metabolic enzymes to detoxify small molecule xenobiotics. It has a complex role in cancer biology, influencing both the progression and suppression of tumors by modulating malignant properties of tumor cells and anti-tumor immunity, depending on the specific tumor type and developmental stage. This has led to the discovery and development of selective AhR modulators, including BAY 2416964 which is currently in clinical trials. To identify small molecule anticancer agents that might be combined with AhR antagonists for cancer therapy, a high-throughput combination screen was performed using multi-cell type tumor spheroids grown from malignant cells, endothelial cells, and mesenchymal stem cells. The AhR selective antagonists BAY 2416964, GNF351, and CH-223191 were tested individually and in combination with twenty-five small molecule anticancer agents. As single agents, BAY 2416964 and CH-223191 showed minimal activity, whereas GNF351 reduced the viability of some spheroid models at concentrations greater than 1 µM. The activity of most combinations aligned well with the single agent without apparent contributions from the AhR antagonist. All three AhR antagonists sensitized tumor spheroids to TAK-243, an E1 ubiquitin-activating enzyme inhibitor. These combinations were active in spheroids containing bladder, breast, ovary, kidney, pancreas, colon, and lung tumor cell lines. The AhR antagonists also potentiated pevonedistat, a selective inhibitor of the NEDD8-activating enzyme E1 regulatory subunit, in several tumor spheroid models. In contrast, the AhR antagonists did not enhance the cytotoxicity of the proteasome inhibitor bortezomib. Copyright © 2024. Published by Elsevier Inc.

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External Sources

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  2. DOI: 10.1016/j.slasd.2024.100186
  3. PMID: 39362362
  4. PII : S2472-5552(24)00048-0

Library Notes

  1. Fiscal Year: FY2024-2025

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