In recent years, immunotherapy has finally found its place in the anti-cancer therapeutic arsenal, even becoming standard of care as first line treatment for metastatic forms. The clinical benefit provided by checkpoint blockers such as anti-PD-1/PD-L1 in many cancers revolutionized the field. However, too many patients remain refractory to these treatments due to weak baseline anti-cancer immunity. There is therefore a need to boost the frequency and function of patients' cytotoxic CD8+ cellular effectors by targeting immunogenic and tumor-restricted antigens, such as neoantigens using an efficient vaccination platform. Dendritic cells (DC) are the most powerful immune cell subset for triggering cellular immune response. However, autologous DC-based vaccines display several limitations, such as the lack of reproducibility and the limited number of cells that can be manufactured. Here we discuss the advantages of a new therapeutic vaccine based on an allogeneic Plasmacytoid DC cell line, which is easy to produce and represents a powerful platform for priming and expanding anti-neoantigen cytotoxic CD8+ T-cells.
Keyphrases
- dendritic cells
- immune response
- regulatory t cells
- end stage renal disease
- newly diagnosed
- ejection fraction
- stem cell transplantation
- chronic kidney disease
- bone marrow
- small cell lung cancer
- peritoneal dialysis
- stem cells
- dna damage
- induced apoptosis
- low dose
- patient reported outcomes
- toll like receptor
- high throughput
- young adults
- papillary thyroid
- single cell
- health insurance
- signaling pathway
- platelet rich plasma
- angiotensin ii