Distinct photo-oxidation-induced cell death pathways lead to selective killing of human breast cancer cells

Author:

Dos Santos Ancély F.,Inague AlexORCID,Arini Gabriel S.,Terra Letícia F.,Wailemann Rosangela A. M.,Pimentel André C.ORCID,Yoshinaga Marcos Y.,Silva Ricardo R.,Severino DivinomarORCID,de Almeida Daria Raquel Q.,Gomes Vinícius M.,Bruni-Cardoso Alexandre,Terra Walter R.,Miyamoto Sayuri,Baptista Maurício S.ORCID,Labriola LeticiaORCID

Abstract

AbstractLack of effective treatments for aggressive breast cancer is still a major global health problem. We have previously reported that photodynamic therapy using methylene blue as photosensitizer (MB-PDT) massively kills metastatic human breast cancer, marginally affecting healthy cells. In this study, we aimed to unveil the molecular mechanisms behind MB-PDT effectiveness and specificity towards tumor cells. Through lipidomics and biochemical approaches, we demonstrated that MB-PDT efficiency and specificity rely on polyunsaturated fatty acid-enriched membranes and on the better capacity to deal with photo-oxidative damage displayed by non-tumorigenic cells. We found out that, in tumorigenic cells, lysosome membrane permeabilization is accompanied by ferroptosis and/or necroptosis. Our results also pointed at a cross-talk between lysosome-dependent cell death (LDCD) and necroptosis induction after photo-oxidation, and contributed to broaden the understanding of MB-PDT-induced mechanisms and specificity in breast cancer cells. Therefore, we demonstrated that efficient approaches could be designed on the basis of lipid composition and metabolic features for hard-to-treat cancers. The results further reinforce MB-PDT as a therapeutic strategy for highly aggressive human breast cancer cells.

Publisher

Springer Science and Business Media LLC

Subject

Cancer Research,Cell Biology,Cellular and Molecular Neuroscience,Immunology

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