pH-Selective Reactions to Selectively Reduce Cancer Cell Proliferation: Effect of CaS Nanostructures in Human Skin Melanoma and Benign Fibroblasts

Olga M Rodríguez Martínez; Michelle A Narváez Ramos; Angeliz A Soto Acevedo; Carolina C Colón Colón; Darlene Malavé Ramos; Coral Castro Rivera; Miguel E Castro Rosario

doi:10.3390/biochem3010002

pH-Selective Reactions to Selectively Reduce Cancer Cell Proliferation: Effect of CaS Nanostructures in Human Skin Melanoma and Benign Fibroblasts

Biochem (Basel). 2023 Mar;3(1):15-30. doi: 10.3390/biochem3010002. Epub 2023 Jan 18.

Authors

Olga M Rodríguez Martínez¹, Michelle A Narváez Ramos¹, Angeliz A Soto Acevedo², Carolina C Colón Colón², Darlene Malavé Ramos¹, Coral Castro Rivera¹, Miguel E Castro Rosario²

Affiliations

¹ Department of Biology, School of Arts and Sciences, University of Puerto Rico at Mayaguez, Mayaguez, PR 00682, USA.
² Department of Chemistry, School of Arts and Sciences, University of Puerto Rico at Mayaguez, Mayaguez, PR 00682, USA.

Abstract

An acidic extracellular pH value (pH_e) is characteristic of many cancers, in contrast to the physiologic pH_e found in most benign cells. This difference in pH offers a unique opportunity to design and engineer chemicals that can be employed for pH-selective reactions in the extracellular fluid of cancer cells. The viability of human skin melanoma and corresponding fibroblasts exposed to CaS dispersions is reported. The viability of melanoma cells decreases with CaS dispersion concentration and reaches 57% at 3%, a value easily distinguishable from melanoma control experiments. In contrast, the viability of benign fibroblasts remains nearly constant within experimental error over the range of dispersion concentrations studied. The CaS dispersions facilitate vinculin delocalization in the cytoplasmic fluid, a result consistent with improved focal adhesion kinase (FAK) regulation in melanoma cells. Thermodynamic considerations are consistent with the formation of $H_{2} S$ from CaS in the presence of protons. The thermodynamic prediction is verified in independent experiments with solid CaS and acidic aqueous solutions. The amount of $H_{2} S$ formed decreases with pH. An activation energy for the process of (30 ± 10) kJ/mol in the temperature range of 280 to 330 K is estimated from initial rate measurements as a function of temperature. The total Gibbs energy minimization approach was employed to establish the distribution of sulfides-including $H_{2} S$ in the gas and aqueous phases-from the dissociation of CaS as a function of pH to mimic physiologically relevant pH values. Theoretical calculations suggest that partially protonated CaS in solution can be stable until the sulfur atom bonds to two hydrogen atoms, resulting in the formation of Ca²⁺ and $H_{2} S$ , which can be solvated and/or released to the gas phase. Our results are consistent with a model in which CaS is dissociated in the extracellular fluid of melanoma cells selectively. The results are discussed in the context of the potential biomedical applications of CaS dispersions in cancer therapies.

Keywords: calcium sulfide nanostructures; extracellular pH; melanoma.

Grants and funding

R25 GM127191/GM/NIGMS NIH HHS/United States