@article{10.1172/jci.insight.132286, author = {Won Jin Ho AND Mark Yarchoan AND Soren Charmsaz AND Rebecca M. Munday AND Ludmila Danilova AND Marcelo B. Sztein AND Elana J. Fertig AND Elizabeth M. Jaffee}, journal = {JCI Insight}, publisher = {The American Society for Clinical Investigation}, title = {Multipanel mass cytometry reveals anti–PD-1 therapy–mediated B and T cell compartment remodeling in tumor-draining lymph nodes}, year = {2020}, month = {1}, volume = {5}, url = {https://insight.jci.org/articles/view/132286}, abstract = {Anti–programmed cell death protein 1 (anti–PD-1) therapy has become an immunotherapeutic backbone for treating many cancer types. Although many studies have aimed to characterize the immune response to anti–PD-1 therapy in the tumor and in the peripheral blood, relatively less is known about the changes in the tumor-draining lymph nodes (TDLNs). TDLNs are primary sites of tumor antigen exposure that are critical to both regulation and cross-priming of the antitumor immune response. We used multipanel mass cytometry to obtain a high-parameter proteomic (39 total unique markers) immune profile of the TDLNs in a well-studied PD-1–responsive, immunocompetent mouse model. Based on combined hierarchal gating and unsupervised clustering analyses, we found that anti–PD-1 therapy enhances remodeling of both B and T cell compartments toward memory phenotypes. Functionally, expression of checkpoint markers was increased in conjunction with production of IFN-γ, TNF-α, or IL-2 in key cell types, including B and T cell subtypes, and rarer subsets, such as Tregs and NKT cells. A deeper profiling of the immunologic changes that occur in the TDLN milieu during effective anti–PD-1 therapy may lead to the discovery of novel biomarkers for monitoring response and provide key insights toward developing combination immunotherapeutic strategies.}, number = {2}, doi = {10.1172/jci.insight.132286}, url = {https://doi.org/10.1172/jci.insight.132286}, }