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Impact of checkpoint blockade on cancer vaccine-activated CD8+ T cell responses.


ABSTRACT: Immune and molecular profiling of CD8 T cells of patients receiving DC vaccines expressing three full-length melanoma antigens (MAs) was performed. Antigen expression levels in DCs had no significant impact on T cell or clinical responses. Patients who received checkpoint blockade before DC vaccination had higher baseline MA-specific CD8 T cell responses but no evidence for improved functional responses to the vaccine. Patients who showed the best clinical responses had low PD-1 expression on MA-specific T cells before and after DC vaccination; however, blockade of PD-1 during antigen presentation by DC had minimal functional impact on PD-1high MA-specific T cells. Gene and protein expression analyses in lymphocytes and tumor samples identified critical immunoregulatory pathways, including CTLA-4 and PD-1. High immune checkpoint gene expression networks correlated with inferior clinical outcomes. Soluble serum PD-L2 showed suggestive positive association with improved outcome. These findings show that checkpoint molecular pathways are critical for vaccine outcomes and suggest specific sequencing of vaccine combinations.

SUBMITTER: Santos PM 

PROVIDER: S-EPMC7336310 | biostudies-literature | 2020 Jul

REPOSITORIES: biostudies-literature

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Impact of checkpoint blockade on cancer vaccine-activated CD8+ T cell responses.

Santos Patricia M PM   Adamik Juraj J   Howes Timothy R TR   Du Samuel S   Vujanovic Lazar L   Warren Sarah S   Gambotto Andrea A   Kirkwood John M JM   Butterfield Lisa H LH  

The Journal of experimental medicine 20200701 7


Immune and molecular profiling of CD8 T cells of patients receiving DC vaccines expressing three full-length melanoma antigens (MAs) was performed. Antigen expression levels in DCs had no significant impact on T cell or clinical responses. Patients who received checkpoint blockade before DC vaccination had higher baseline MA-specific CD8 T cell responses but no evidence for improved functional responses to the vaccine. Patients who showed the best clinical responses had low PD-1 expression on MA  ...[more]

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