TY - JOUR
T1 - An Immunogenic Model of KRAS-Mutant Lung Cancer Enables Evaluation of Targeted Therapy and Immunotherapy Combinations
AU - Boumelha, Jesse
AU - de Carné Trécesson, Sophie
AU - Law, Emily K.
AU - Romero-Clavijo, Pablo
AU - Coelho, Matthew A.
AU - Ng, Kevin W.
AU - Mugarza, Edurne
AU - Moore, Christopher
AU - Rana, Sareena
AU - Caswell, Deborah R.
AU - Murillo, Miguel
AU - Hancock, David C.
AU - Argyris, Prokopios P.
AU - Brown, William L.
AU - Durfee, Cameron
AU - Larson, Lindsay K.
AU - Vogel, Rachel I.
AU - Suárez-Bonnet, Alejandro
AU - Priestnall, Simon L.
AU - East, Philip
AU - Ross, Sarah J.
AU - Kassiotis, George
AU - Molina-Arcas, Miriam
AU - Swanton, Charles
AU - Harris, Reuben
AU - Downward, Julian
N1 - Publisher Copyright:
©2022 American Association for Cancer Research.
PY - 2022/10/1
Y1 - 2022/10/1
N2 - Mutations in oncogenes such as KRAS and EGFR cause a high proportion of lung cancers. Drugs targeting these proteins cause tumor regression but ultimately fail to elicit cures. As a result, there is an intense interest in how to best combine targeted therapies with other treatments, such as immunotherapies. However, preclinical systems for studying the interaction of lung tumors with the host immune system are inadequate, in part due to the low tumor mutational burden in genetically engineered mouse models. Here we set out to develop mouse models of mutant KRAS–driven lung cancer with an elevated tumor mutational burden by expressing the human DNA cytosine deaminase, APOBEC3B, to mimic the mutational signature seen in human lung cancer. This failed to substantially increase clonal tumor mutational burden and autochthonous tumors remained refractory to immunotherapy. However, establishing clonal cell lines from these tumors enabled the generation of an immunogenic syngeneic transplantation model of KRAS-mutant lung adenocarcinoma that was sensitive to immunotherapy. Unexpectedly, antitumor immune responses were not directed against neoantigens but instead targeted derepressed endogenous retroviral antigens. The ability of KRASG12C inhibitors to cause regression of KRASG12C -expressing tumors was markedly potentiated by the adaptive immune system, highlighting the importance of using immunocompetent models for evaluating targeted therapies. Overall, this model provides a unique opportunity for the study of combinations of targeted and immunotherapies in immune-hot lung cancer.
AB - Mutations in oncogenes such as KRAS and EGFR cause a high proportion of lung cancers. Drugs targeting these proteins cause tumor regression but ultimately fail to elicit cures. As a result, there is an intense interest in how to best combine targeted therapies with other treatments, such as immunotherapies. However, preclinical systems for studying the interaction of lung tumors with the host immune system are inadequate, in part due to the low tumor mutational burden in genetically engineered mouse models. Here we set out to develop mouse models of mutant KRAS–driven lung cancer with an elevated tumor mutational burden by expressing the human DNA cytosine deaminase, APOBEC3B, to mimic the mutational signature seen in human lung cancer. This failed to substantially increase clonal tumor mutational burden and autochthonous tumors remained refractory to immunotherapy. However, establishing clonal cell lines from these tumors enabled the generation of an immunogenic syngeneic transplantation model of KRAS-mutant lung adenocarcinoma that was sensitive to immunotherapy. Unexpectedly, antitumor immune responses were not directed against neoantigens but instead targeted derepressed endogenous retroviral antigens. The ability of KRASG12C inhibitors to cause regression of KRASG12C -expressing tumors was markedly potentiated by the adaptive immune system, highlighting the importance of using immunocompetent models for evaluating targeted therapies. Overall, this model provides a unique opportunity for the study of combinations of targeted and immunotherapies in immune-hot lung cancer.
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U2 - 10.1158/0008-5472.CAN-22-0325
DO - 10.1158/0008-5472.CAN-22-0325
M3 - Article
C2 - 35930804
AN - SCOPUS:85139570458
SN - 0008-5472
VL - 82
SP - 3435
EP - 3448
JO - Cancer Research
JF - Cancer Research
IS - 19
ER -