Investigation of cell death mechanisms in human lymphatic endothelial cells undergoing photodynamic therapy

Background: Photodynamic therapy (PDT) has been shown to induce ablation and functional occlusion of tumor-associated lymphatic vessels. However, direct effects of PDT on lymphatic endothelial cells (LECs) have not been studied so far. The aim of this study was to elucidate molecular mechanisms of cell death induced by PDT in human LECs. Methods: Verteporfin was used as a photosensitizer to investigate PDT-mediated damage of lymphatic vessels in mice using immunofluorescent staining and stereomicroscopy. In vitro dose-response studies were carried-out with crystal violet staining. Immunofluorescence, flow cytometry, immunoblotting and DNA electrophoresis were used to investigate the mechanisms of cell death in human LECs undergoing PDT. Results: PDT induced an increase in the number of propidium iodide positive lymphatic endothelial cells in the mouse dermis. In in vitro studies dose-dependent cytotoxic effects of PDT towards LECs were observed. Typical hallmarks of apoptotic cell death, including Annexin V binding, loss of mitochondrial membrane potential, caspase activation, cleavage of PARP as well as DNA fragmentation were observed in LECs when PDT was used at high irradiation conditions, causing >80% cell death. At lower light fluencies causing

Investigation of cell death mechanisms in human lymphatic endothelial cells undergoing photodynamic therapy

Colon tumour cell death causes mTOR dependence by paracrine P2X4 stimulation

In vitro endoderm emergence and self-organisation in the absence of extraembryonic tissues and embryonic architecture

In vitro endoderm emergence and self-organisation in the absence of extraembryonic tissues and embryonic architecture

Colon tumour cell death causes mTOR dependence by paracrine P2X4 stimulation