AI Article Synopsis
- Antigen cross-presentation is vital for activating CD8 T cells in antitumor immune responses, with dendritic cells (DCs) loaded with tumor antigens showing promise in clinical trials.
- Researchers treated mice with dead tumor cells expressing the fusogenic protein from the infectious salmon anemia virus (ISAV), which enhanced dendritic cell maturation and antigen transfer.
- In melanoma models, both types of dead tumor cells reduced tumor growth, but only those expressing the ISAV fusion protein increased CD4 and CD8 T cell populations in the spleen, indicating potential for improving cancer treatments.
Article Abstract
Antigen cross-presentation is a crucial step in the assembly of an antitumor immune response leading to activation of naïve CD8 T cells. This process has been extensively used in clinical trials, in which dendritic cells generated are loaded with tumor antigens and then autotransplanted to the patients. Recently, the use of autologous transplant of dendritic cells fused with dying tumor cells has demonstrated good results in clinical studies. In this work, we generated a similar process by treating mice with dead tumor cells [cell bodies (CBs)] expressing the fusogenic protein of the infectious salmon anemia virus (ISAV). ISAV fusion protein retains its fusogenic capability when is expressed on mammalian cells and the CBs expressing it facilitates DCs maturation, antigen transfer by antigen-presenting cells, and increase cross-presentation by DCs . Additionally, we observed in the melanoma model that CBs with or without ISAV fusion protein reduce tumor growth in prophylactic treatment; however, only ISAV expressing CBs showed an increase CD4 and CD8 cells in spleen. Overall, our results suggest that CBs could be used as a complement with other type of strategies to amplify antitumor immune response.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5640808 | PMC |
| http://dx.doi.org/10.3389/fimmu.2017.01170 | DOI Listing |
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