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Peer-reviewed veterinary case report

HDAC/σ1R Dual-Ligand as a Targeted Melanoma Therapeutic.

Year:
2025
Authors:
Leotta CG et al.
Affiliation:
Dream Factory Lab · Italy

Abstract

<b>Background:</b> In melanoma, multiligand drug strategies to disrupt cancer-associated epigenetic alterations and angiogenesis are particularly promising. Here, a novel dual-ligand with a single shared pharmacophore capable of simultaneously targeting histone deacetylases (HDACs) and sigma receptors (σRs) was synthesized and subjected to phenotypic in vitro screening. <b>Methods</b>: Tumor cell proliferation and spreading were investigated using immortalized human cancer and normal cell lines. Angiogenesis was also evaluated in mouse endothelial cells using a tube formation assay. <b>Results:</b> The dual-ligand compound exhibited superior potency in suppressing both uveal and cutaneous melanoma cell viability compared to other cancer cell types or normal cells. Melanoma selectivity reflected inhibition of the HDAC-dependent epigenetic regulation of tumor proliferative kinetics, without involvement of σR signaling. In contrast, the bifunctional compound inhibited the formation of capillary-like structures, formed by endothelial cells, and tumor cell spreading through the specific regulation of σ<sub>1</sub>R signaling, but not HDAC activity. <b>Conclusions:</b> Together, the present findings suggest that dual-targeted HDAC/σ<sub>1</sub>R ligands might efficiently and simultaneously disrupt tumor growth, dissemination and angiogenesis in melanoma, a strategy amenable to future clinical applications in precision cancer treatment.

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Original publication: https://europepmc.org/article/MED/40005993