Medizinische Universität Graz Austria/Österreich - Forschungsportal - Medical University of Graz

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SHR Neuro Krebs Kardio Lipid Stoffw Microb

Dengler, MA; Teh, CE; Thijssen, R; Gangoda, L; Lan, P; Herold, MJ; Gray, DH; Kelly, GL; Roberts, AW; Adams, JM.
Potent efficacy of MCL-1 inhibitor-based therapies in preclinical models of mantle cell lymphoma.
Oncogene. 2020; 39(9):2009-2023 Doi: 10.1038/s41388-019-1122-x
Web of Science PubMed FullText FullText_MUG

Führende Autor*innen der Med Uni Graz: Dengler Michael
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Abstract:: Apoptosis-regulating BCL-2 family members, which can promote malignant transformation and resistance to therapy, have become prime therapeutic targets, as illustrated by the striking efficacy in certain lymphoid malignancies of the BCL-2-specific inhibitor venetoclax. In other lymphoid malignancies, however, such as the aggressive mantle cell lymphoma (MCL), cell survival might rely instead or also on BCL-2 relative MCL-1. We have explored MCL-1 as a target for killing MCL cells by both genetic and pharmacologic approaches. In several MCL cell lines, MCL-1 knockout with an inducible CRISPR/Cas9 system triggered spontaneous apoptosis. Accordingly, most MCL cell lines proved sensitive to the specific MCL-1 inhibitor S63845, and MCL-1 inhibition also proved efficacious in an MCL xenograft model. Furthermore, its killing efficacy rose on combination with venetoclax, the BCL-X_L-specific inhibitor A-1331852, or Bruton's tyrosine kinase (BTK) inhibitor ibrutinib, which reduced pro-survival signals. We also tested the MCL-1 inhibitor in primary samples from 13 MCL patients, using CD40L-expressing feeder cells to model their microenvironmental support. Notably, all unstimulated primary MCL samples were very sensitive to S63845, but the CD40L stimulation attenuated their sensitivity. Mass cytometric analysis revealed that the stimulation likely conveyed protection by elevating BCL-X_L and MCL-1. Accordingly, sensitivity of the CD40L-stimulated cells to S63845 was substantially restored by co-treatment with venetoclax, the BCL-X_L-specific inhibitor or ibrutinib. Overall, our findings indicate that MCL-1 is very important for survival of MCL cells and that the MCL-1 inhibitor, both alone and together with ibrutinib, venetoclax or a BCL-X_L inhibitor, offers promise for novel improved MCL therapies.
Find related publications in this database (using NLM MeSH Indexing): Animals -; Antineoplastic Agents - pharmacology; Apoptosis -; Bridged Bicyclo Compounds, Heterocyclic - pharmacology; Cell Proliferation -; Humans -; Lymphoma, Mantle-Cell - drug therapy; Lymphoma, Mantle-Cell - metabolism; Lymphoma, Mantle-Cell - pathology; Mice -; Mice, Inbred NOD -; Mice, SCID -; Myeloid Cell Leukemia Sequence 1 Protein - antagonists & inhibitors; Pyrimidines - pharmacology; Sulfonamides - pharmacology; Thiophenes - pharmacology; Tumor Cells, Cultured -; Xenograft Model Antitumor Assays -; bcl-X Protein - antagonists & inhibitors