Mismatch repair deficiency is not sufficient to elicit tumor immunogenicity-Reference-Cited by-同舟云学术

Mismatch repair deficiency is not sufficient to elicit tumor immunogenicity

Published:2023-09-14 Issue:10 Volume:55 Page:1686-1695
ISSN:1061-4036
Container-title:Nature Genetics
language:en
Short-container-title:Nat Genet

Author:

Westcott Peter M. K.^ORCID,Muyas Francesc,Hauck Haley,Smith Olivia C.^ORCID,Sacks Nathan J.,Ely Zackery A.,Jaeger Alex M.,Rideout William M.,Zhang Daniel^ORCID,Bhutkar Arjun,Beytagh Mary C.^ORCID,Canner David A.,Jaramillo Grissel C.,Bronson Roderick T.,Naranjo Santiago,Jin Abbey,Patten J. J.^ORCID,Cruz Amanda M.,Shanahan Sean-Luc,Cortes-Ciriano Isidro^ORCID,Jacks Tyler^ORCID

Abstract

AbstractDNA mismatch repair deficiency (MMRd) is associated with a high tumor mutational burden (TMB) and sensitivity to immune checkpoint blockade (ICB) therapy. Nevertheless, most MMRd tumors do not durably respond to ICB and critical questions remain about immunosurveillance and TMB in these tumors. In the present study, we developed autochthonous mouse models of MMRd lung and colon cancer. Surprisingly, these models did not display increased T cell infiltration or ICB response, which we showed to be the result of substantial intratumor heterogeneity of mutations. Furthermore, we found that immunosurveillance shapes the clonal architecture but not the overall burden of neoantigens, and T cell responses against subclonal neoantigens are blunted. Finally, we showed that clonal, but not subclonal, neoantigen burden predicts ICB response in clinical trials of MMRd gastric and colorectal cancer. These results provide important context for understanding immune evasion in cancers with a high TMB and have major implications for therapies aimed at increasing TMB.

Publisher

Springer Science and Business Media LLC

Subject

Genetics

Link

https://www.nature.com/articles/s41588-023-01499-4.pdf

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