Repurposed clindamycin suppresses pyroptosis in tumor-associated macrophages through Inhibition of caspase-1

Weich, Adrian; Berges, Johannes; Flamann, Cindy; Bitterer, Katrin; Singh, Krishna Pal; Chambers, David; Lischer, Christopher; Lai, Xin; Wolkenhauer, Olaf; Berking, Carola; Krönke, Gerhard; Gupta, Shailendra; Bruns, Heiko; Vera, Julio; Macrophages, Research Group

Repurposed clindamycin suppresses pyroptosis in tumor-associated macrophages through Inhibition of caspase-1

Weich, Adrian; Berges, Johannes; Flamann, Cindy; Bitterer, Katrin; Singh, Krishna Pal; Chambers, David; Lischer, Christopher; Lai, Xin; Wolkenhauer, Olaf; Berking, Carola; Krönke, Gerhard; Gupta, Shailendra; Bruns, Heiko; Vera, Julio; Macrophages, Research Group (2025)

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s13046-025-03478-5.pdf (5.032Mt)

Lataukset:

Weich, Adrian

Berges, Johannes

Flamann, Cindy

Bitterer, Katrin

Singh, Krishna Pal

Chambers, David

Lischer, Christopher

Lai, Xin

Wolkenhauer, Olaf

Berking, Carola

Krönke, Gerhard

Gupta, Shailendra

Bruns, Heiko

Vera, Julio

Macrophages, Research Group

2025

Journal of Experimental and Clinical Cancer Research
225

doi:10.1186/s13046-025-03478-5

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Julkaisun pysyvä osoite on
https://urn.fi/URN:NBN:fi:tuni-202510149895

Kuvaus

Peer reviewed

Tiivistelmä

Background: The metastatic microenvironment is often rich in tumor-associated macrophages (TAMs). In uveal melanoma (UM), high levels of TAMs positively correlate with tumor progression and poorer prognosis. We hypothesize that the immunomodulation of TAMs can remodel the UM tumor microenvironment and make it more susceptible to therapeutic interventions. Methods: In our work, we designed a novel computational pipeline that combines single-cell transcriptomics data, network analysis, multicriteria decision techniques, and pharmacophore-based docking simulations to select molecular targets and matching repurposable drugs for TAM immunomodulation. The method generates a ranking of drug-target interactions, the most promising of which are channeled towards experimental validation. Results: To identify potential immunomodulatory targets, we created a network-based representation of the TAM interactome and extracted a regulatory core conditioned on UM expression data. Further, we selected 13 genes from this core (NLRP3, HMOX1, CASP1, GSTP1, NAMPT, HSP90AA1, B2M, ISG15, LTA4H, PTGS2, CXCL2, PLAUR, ZFP36, TANK) for pharmacophore-based virtual screening of FDA-approved compounds, followed by flexible molecular docking. Based on the ranked docking results, we chose the interaction between caspase-1 and clindamycin for experimental validation. Functional studies on macrophages confirmed that clindamycin inhibits caspase-1 activity and thereby inflammasome activation, leading to a decrease in IL-1β, IL-18, and gasdermin D cleavage products as well as a reduction in pyroptotic cell death. This clindamycin-mediated inhibition of caspase-1 was also observable in TAMs derived from the bone marrow of multiple myeloma patients. Conclusions: Our computational workflow for drug repurposing identified clindamycin as an efficacious inhibitor of caspase-1 that suppresses inflammasome activity and pyroptosis in vitro in TAMs.

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TUNICRIS-julkaisut [24324]