4.3 Article

Sigma-1 and Sigma-2 receptor ligands induce apoptosis and autophagy but have opposite effect on cell proliferation in uveal melanoma

Journal

ONCOTARGET
Volume 8, Issue 53, Pages 91099-91111

Publisher

IMPACT JOURNALS LLC
DOI: 10.18632/oncotarget.19556

Keywords

uveal melanoma; sigma receptors; apoptosis; autophagy; (+)-pentazocine

Funding

  1. Fondazione Mani Amiche Onlus (Catania, Italy)
  2. University of Catania (Catania, Italy) [FIR2014]

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Uveal melanoma is the most common primary intraocular tumor in adults, with about 1200-1500 new cases occurring per year in the United States. Metastasis is a frequent occurrence in uveal melanoma, and outcomes are poor once distant spread occurs and no clinically significant chemotherapeutic protocol is so far available. The aim of the present study was to test the effect of various sigma 1 and sigma 2 receptor ligands as a possible pharmacological strategy for this rare tumor. Human uveal melanoma cells (92.1) were treated with various concentrations of different s2 ligands (haloperidol and haloperidol metabolite II) and s1 ligand ((+)-pentazocine) at various concentrations (1, 10 and 25 mu M) and time points (0, 4 h, 8 h, 24 h and 48 h). Cell proliferation and migration were evaluated respectively by continuous cell monitoring by xCELLigence analysis, clonogenic assay and wound healing. Apoptosis and autophagy were also measured by cytofluorimetric and microscopy analysis. Our results showed that s2 receptor ligands significantly reduced cell proliferation whereas (+)-pentazocine exhibited opposite results. All tested ligands showed significant decrease in cell migration. Interestingly, both s1 and s2 receptor ligands showed significant increase of autophagy and apoptosis at all concentrations. Taken all together these results suggest that sigma receptors mediates opposite biological effects but they also share common pharmacological effect on apoptosis and autophagy in uveal melanoma. In conclusion, these data provide the first evidence that sigma receptors may represent a druggable target to develop new chemotherapic agent for uveal melanoma.

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