A PoleP286R mouse model of endometrial cancer recapitulates high mutational burden and immunotherapy response
Hao-Dong Li, Changzheng Lu, He Zhang, Qing Hu, Junqiu Zhang, Ileana C. Cuevas, Subhransu S. Sahoo, Mitzi Aguilar, Elizabeth G. Maurais, Shanrong Zhang, Xiaojing Wang, Esra A. Akbay, Guo-Min Li, Bo Li, Prasad Koduru, Peter Ly, Yang-Xin Fu, Diego H. Castrillon
Hao-Dong Li, Changzheng Lu, He Zhang, Qing Hu, Junqiu Zhang, Ileana C. Cuevas, Subhransu S. Sahoo, Mitzi Aguilar, Elizabeth G. Maurais, Shanrong Zhang, Xiaojing Wang, Esra A. Akbay, Guo-Min Li, Bo Li, Prasad Koduru, Peter Ly, Yang-Xin Fu, Diego H. Castrillon
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Research Article Genetics Oncology

A PoleP286R mouse model of endometrial cancer recapitulates high mutational burden and immunotherapy response

Abstract

Cancer is instigated by mutator phenotypes, including deficient mismatch repair and p53-associated chromosomal instability. More recently, a distinct class of cancers was identified with unusually high mutational loads due to heterozygous amino acid substitutions (most commonly P286R) in the proofreading domain of DNA polymerase ε, the leading strand replicase encoded by POLE. Immunotherapy has revolutionized cancer treatment, but new model systems are needed to recapitulate high mutational burdens characterizing human cancers and permit study of mechanisms underlying clinical responses. Here, we show that activation of a conditional LSL-PoleP286R allele in endometrium is sufficient to elicit in all animals endometrial cancers closely resembling their human counterparts, including very high mutational burden. Diverse investigations uncovered potentially novel aspects of Pole-driven tumorigenesis, including secondary p53 mutations associated with tetraploidy, and cooperation with defective mismatch repair through inactivation of Msh2. Most significantly, there were robust antitumor immune responses with increased T cell infiltrates, accelerated tumor growth following T cell depletion, and unfailing clinical regression following immune checkpoint therapy. This model predicts that human POLE-driven cancers will prove consistently responsive to immune checkpoint blockade. Furthermore, this is a robust and efficient approach to recapitulate in mice the high mutational burdens and immune responses characterizing human cancers.

Authors

Hao-Dong Li, Changzheng Lu, He Zhang, Qing Hu, Junqiu Zhang, Ileana C. Cuevas, Subhransu S. Sahoo, Mitzi Aguilar, Elizabeth G. Maurais, Shanrong Zhang, Xiaojing Wang, Esra A. Akbay, Guo-Min Li, Bo Li, Prasad Koduru, Peter Ly, Yang-Xin Fu, Diego H. Castrillon

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Figure 6

Acceleration of tumor progression following T cell depletion.

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Acceleration of tumor progression following T cell depletion. (A) CD3 IH...
(A) CD3 IHC highlighting T cells, normal uterus versus tumor, with slides counterstained with hematoxylin. Scale bars: 25 μm. (B) Schematic summarizing CD8+ T cell depletion protocol. (C) αCD8 antibody resulted in near total CD8+ T cell depletion (inset boxes) in peripheral blood sampled 6 days after the first CD8 antibody injection. x axis, allophycocyanin-stained CD8; y axis, phycoerythrin-stained CD3ε. (D) IHC of CD8+ T cells in splenic tissue shows systemic tissue depletion. Tissue obtained 3 days after 27 weeks of treatment. Scale bars: 40 μm. (EG) Mice euthanized after 27-week interval as shown in C. (E) MRI and matching gross images of uteri, from representative control and experimentally treated mice. Scale bars: 0.5 cm. (F) Uterus weights in control (n = 6) versus treated mice (n = 7), P value per 2-tailed Mann-Whitney U test. (G) Tumor burden per weight measurements likely underestimates overall tumor extent. White arrows show histologic extent of tumors. Scale bars: 250 μm.