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2B4 but not PD-1 blockade improves mortality in septic animals with preexisting malignancy
Ching-wen Chen, … , Craig M. Coopersmith, Mandy L. Ford
Ching-wen Chen, … , Craig M. Coopersmith, Mandy L. Ford
Published November 14, 2019
Citation Information: JCI Insight. 2019;4(22):e127867. https://doi.org/10.1172/jci.insight.127867.
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Research Article Immunology

2B4 but not PD-1 blockade improves mortality in septic animals with preexisting malignancy

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Abstract

In addition to its well-known beneficial effects for the treatment of several types of cancer, PD-1 blockade has shown encouraging results in preclinical models of sepsis and in a recent clinical trial in sepsis. Because cancer is the most common comorbidity in septic patients, here we aimed to determine the efficacy of PD-1 checkpoint blockade in the setting of sepsis complicated with preexisting malignancy. In a model of established lung cancer followed by cecal ligation and puncture–induced (CLP-induced) sepsis, PD-1 blockade exhibited no therapeutic effect on sepsis survival. This diminished efficacy of PD-1 blockade in cancer septic animals (septic animals with cancer) was characterized by a reduction in both the quality and quantity of PD-1+ responder cells. Specifically, CD8+ T cells isolated from cancer septic animals exhibited decreased CD28 expression and a reduction in the CXCR5+PD-1+ subset. In addition, flow cytometric analysis of T cells isolated from cancer septic animals revealed 2B4 as another possible checkpoint under these conditions. Administration of anti-2B4 to cancer septic animals significantly improved sepsis survival and was associated with increased T cell costimulatory receptor expression and decreased coinhibitory receptor expression. These results illustrate functions of coinhibitory receptors in the setting of sepsis complicated with cancer.

Authors

Ching-wen Chen, Ming Xue, Wenxiao Zhang, Jianfeng Xie, Craig M. Coopersmith, Mandy L. Ford

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Figure 5

CITRUS identifies similar CD8+ populations that are elevated in cancer septic animals.

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CITRUS identifies similar CD8+ populations that are elevated in cancer s...
The CD8+ data sets described in Figure 4 were exported into the CITRUS algorithm (Cytobank) and PAMR association model with minimum FDR was selected. (A) Plots of abundance and significantly changed clusters were automatically generated by CITRUS. (B) The abundance summary plot of nodes that were significantly different between previously healthy (PH) cecal ligation and puncture (CLP) and cancer (CA) CLP groups. (C) Phenotype histograms of the nodes that are increased in cancer septic animals. n = 10–11.

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