Reverse Translating Molecular Determinants of Anti-Programmed Death 1 Immunotherapy Response in Mouse Syngeneic Tumor Models.

Peter Georgiev,Louise Cadzow,Mingmei Cai,Derek Y Chiang,Michael Nebozhyn,Manjiri Sathe,Marlene C Hinton,Heather A Hirsch,Svetlana Sadekova,Selvakumar Sukumar,Michael Caniga,Hui Xiao,Wendy M Blumenschein,Terrill K Mcclanahan,Venkataraman Sriram,Jennifer H Yearley,Brian J Long,Sarah Javaid,Eric S Muise,Lily Y Moy,Andrey Loboda,Elaine M Pinheiro,Yun Wang,Lan Chen,Douglas C Wilson,Aleksandra Olow ,Douglas E Linn ,Kimberly S Kerr ,Răzvan Cristescu

doi:10.1158/1535-7163.mct-21-0561

Peter Georgiev, Louise Cadzow + Show 27 more

Open Access

https://doi.org/10.1158/1535-7163.mct-21-0561

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Abstract

Targeting the programmed death 1/programmed death ligand 1 (PD-1/PD-L1) pathway with immunotherapy has revolutionized the treatment of many cancers. Somatic tumor mutational burden (TMB) and T-cell-inflamed gene expression profile (GEP) are clinically validated pan-tumor genomic biomarkers that can predict responsiveness to anti-PD-1/PD-L1 monotherapy in many tumor types. We analyzed the association between these biomarkers and the efficacy of PD-1 inhibitor in 11 commonly used preclinical syngeneic tumor mouse models using murinized rat anti-mouse PD-1 DX400 antibody muDX400, a surrogate for pembrolizumab. Response to muDX400 treatment was broadly classified into three categories: highly responsive, partially responsive, and intrinsically resistant to therapy. Molecular and cellular profiling validated differences in immune cell infiltration and activation in the tumor microenvironment of muDX400-responsive tumors. Baseline and on-treatment genomic analysis showed an association between TMB, murine T-cell-inflamed gene expression profile (murine-GEP), and response to muDX400 treatment. We extended our analysis to investigate a canonical set of cancer and immune biology-related gene signatures, including signatures of angiogenesis, myeloid-derived suppressor cells, and stromal/epithelial-to-mesenchymal transition/TGFβ biology previously shown to be inversely associated with the clinical efficacy of immune checkpoint blockade. Finally, we evaluated the association between murine-GEP and preclinical efficacy with standard-of-care chemotherapy or antiangiogenic agents that previously demonstrated promising clinical activity, in combination with muDX400. Our profiling studies begin to elucidate the underlying biological mechanisms of response and resistance to PD-1/PD-L1 blockade represented by these models, thereby providing insight into which models are most appropriate for the evaluation of orthogonal combination strategies.

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