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Endogenous T cell responses to antigens expressed in lung adenocarcinomas delay malignant tumor progression.


ABSTRACT: Neoantigens derived from somatic mutations in tumors may provide a critical link between the adaptive immune system and cancer. Here, we describe a system to introduce exogenous antigens into genetically engineered mouse lung cancers to mimic tumor neoantigens. We show that endogenous T cells respond to and infiltrate tumors, significantly delaying malignant progression. Despite continued antigen expression, T cell infiltration does not persist and tumors ultimately escape immune attack. Transplantation of cell lines derived from these lung tumors or prophylactic vaccination against the autochthonous tumors, however, results in rapid tumor eradication or selection of tumors that lose antigen expression. These results provide insight into the dynamic nature of the immune response to naturally arising tumors.

SUBMITTER: DuPage M 

PROVIDER: S-EPMC3069809 | biostudies-literature | 2011 Jan

REPOSITORIES: biostudies-literature

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Endogenous T cell responses to antigens expressed in lung adenocarcinomas delay malignant tumor progression.

DuPage Michel M   Cheung Ann F AF   Mazumdar Claire C   Winslow Monte M MM   Bronson Roderick R   Schmidt Leah M LM   Crowley Denise D   Chen Jianzhu J   Jacks Tyler T  

Cancer cell 20110101 1


Neoantigens derived from somatic mutations in tumors may provide a critical link between the adaptive immune system and cancer. Here, we describe a system to introduce exogenous antigens into genetically engineered mouse lung cancers to mimic tumor neoantigens. We show that endogenous T cells respond to and infiltrate tumors, significantly delaying malignant progression. Despite continued antigen expression, T cell infiltration does not persist and tumors ultimately escape immune attack. Transpl  ...[more]

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