TIGIT modulates sepsis-induced immune dysregulation in mice with preexisting malignancy
Wenxiao Zhang, Jerome C. Anyalebechi, Kimberly M. Ramonell, Ching-wen Chen, Jianfeng Xie, Zhe Liang, Deena B. Chihade, Shunsuke Otani, Craig M. Coopersmith, Mandy L. Ford
Wenxiao Zhang, Jerome C. Anyalebechi, Kimberly M. Ramonell, Ching-wen Chen, Jianfeng Xie, Zhe Liang, Deena B. Chihade, Shunsuke Otani, Craig M. Coopersmith, Mandy L. Ford
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Research Article Immunology Inflammation

TIGIT modulates sepsis-induced immune dysregulation in mice with preexisting malignancy

Abstract

TIGIT is a recently identified coinhibitory receptor that is upregulated in the setting of cancer and functionally contributes to the impairment of antitumor immunity. However, its role during sepsis is unknown. Because patients with cancer are 10 times more likely to die of sepsis than previously healthy (PH) patients with sepsis, we interrogated the role of TIGIT during sepsis in the context of preexistent malignancy. PH mice or cancer (CA) mice inoculated with lung carcinoma cells were made septic by cecal ligation and puncture (CLP). We found that sepsis induced TIGIT upregulation predominantly on Tregs and NK cells in both PH and CA mice. Anti-TIGIT Ab improved the 7-d survival of CA septic mice but not PH mice after CLP. Treatment of CA septic animals but not PH septic animals with anti-TIGIT mAb significantly reversed sepsis-induced loss of CD4+ T cells, CD8+ T cells, Foxp3+ Treg, and CD19+ B cells in the spleen, which was the result of decreased caspase-3+ apoptotic cells. In sum, we found that anti-TIGIT Ab reversed sepsis-induced T cell apoptosis in CA septic mice and led to a significant survival benefit, suggesting its use as a potential immunotherapy to improve outcomes in septic patients with cancer.

Authors

Wenxiao Zhang, Jerome C. Anyalebechi, Kimberly M. Ramonell, Ching-wen Chen, Jianfeng Xie, Zhe Liang, Deena B. Chihade, Shunsuke Otani, Craig M. Coopersmith, Mandy L. Ford

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Figure 1

TIGIT is upregulated on splenic lymphocytes isolated from PH septic mice and septic mice with preexisting malignancy (CA).

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TIGIT is upregulated on splenic lymphocytes isolated from PH septic mice...
B6 mice were injected with LLC and monitored for 3 weeks. PH and CA mice were subjected to CLP (n = 22/group) or sham surgery (n = 5/group). Mice were sacrificed on days 1, 2, and 3 after CLP and TIGIT expression on splenic immune cells was measured. (A and C) Representative flow histograms showing TIGIT expression on the indicated lymphocyte populations isolated from either PH or CA septic mice. Plots were gated on CD4+, CD4+Foxp3+/–, CD8+, NK1.1+, and CD19+ cells, respectively. (B and D) Summary data of the percentage of TIGIT+ lymphocytes isolated from either PH or CA septic mice. (E) TIGIT expression on each cell subset was compared between PH and CA mice at different time points. Groups were compared with 2-way ANOVA with Tukey’s post hoc test. *P ≤ 0.05, **P ≤ 0.01, ***P ≤ 0.001. PH, previously healthy; CA, cancer; LLC, Lewis lung carcinoma; CLP, cecal ligation and puncture; TIGIT, T cell Ig and ITIM domain.