OX40 expression in neutrophils promotes hepatic ischemia/reperfusion injury
Hua Jin, Chunpan Zhang, Chengyang Sun, Xinyan Zhao, Dan Tian, Wen Shi, Yue Tian, Kai Liu, Guangyong Sun, Hufeng Xu, Dong Zhang
Hua Jin, Chunpan Zhang, Chengyang Sun, Xinyan Zhao, Dan Tian, Wen Shi, Yue Tian, Kai Liu, Guangyong Sun, Hufeng Xu, Dong Zhang
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Research Article Hepatology Transplantation

OX40 expression in neutrophils promotes hepatic ischemia/reperfusion injury

Abstract

Neutrophils play critical roles during the initial phase of hepatic ischemia/reperfusion injury (HIRI). However, the regulation of neutrophil activation, infiltration, and proinflammatory cytokine secretion has not been fully elucidated. In this study, we revealed that OX40 was expressed by neutrophils, its expression in neutrophils was time-dependently upregulated following HIRI, and Ox40 knockout markedly alleviated liver injury. Compared with wild-type neutrophils, the adoptive transfer of Ox40–/– neutrophils decreased HIRI in neutrophil-depleted Rag2/Il2rg–/– or Ox40–/– mice. Moreover, consistently, the in vitro experiments showed that Ox40 not only prolonged neutrophil survival but also promoted proinflammatory cytokines, ROS production, and even neutrophil chemotaxis. Further investigation demonstrated that the knockout of Ox40 in neutrophils inhibited NF-κB signaling via the TRAF1/2/4 and IKKα/IKKβ/IκBα pathways. OX40L and OX86 stimulation could enhance neutrophil activation and survival in vitro and in vivo. In conclusion, our study provides a new understanding of OX40, which is expressed not only in adaptive immune cells but also in innate immune cells, i.e., neutrophils, contributing to the activation and survival of neutrophils. These findings provide a novel potential therapeutic target for the prevention of HIRI during liver transplantation or hepatic surgery.

Authors

Hua Jin, Chunpan Zhang, Chengyang Sun, Xinyan Zhao, Dan Tian, Wen Shi, Yue Tian, Kai Liu, Guangyong Sun, Hufeng Xu, Dong Zhang

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Figure 1

HIRI peaked after 6 hours of reperfusion and mediated the upregulation of OX40 expression in neutrophils.

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HIRI peaked after 6 hours of reperfusion and mediated the upregulation o...
(A) Serum ALT levels following 1 hour of ischemia and different reperfusion times (1 hour, 2 hours, 4 hours, 6 hours, 12 hours, 24 hours, 48 hours, and 72 hours after reperfusion) were examined (n = 3/group). (B) CD45+ leukocytes were gated for an analysis of the neutrophil (Ly6G+ and CD11b+ subsets) proportions at different time points (1 hour, 2 hours, 4 hours, 6 hours, and 8 hours after reperfusion), and the neutrophils were characterized by flow cytometry (n = 3–5/group). (C) Statistical analysis of neutrophil proportions in CD45+ gates (n = 3–5/group). Neutrophils were isolated from liver mononuclear cells (MNCs) by FACS after different reperfusion times, and relative mRNA expression of Ox40 (D) was measured by real-time PCR (n = 5/group). Representative flow cytometric results (E) and statistical analysis (F) of OX40 expression in neutrophils (CD45+Ly6G+CD11b+ subsets) (n = 5/group). (G) Relative MFI levels of OX40 in neutrophils plotted in each group (n = 5/group). Neutrophils were isolated from liver MNCs by FACS after different reperfusion times, and relative mRNA expression of Tnfa (H) and Il1b (I) was measured by real-time PCR (n = 5/group). Serum TNF-α (J) and IL-1β (K) levels (pg/mL) were measured by mouse inflammation panel (n = 5/group). Data represent mean ± SD. Significant differences were analyzed using 2-tailed Student’s t test and 1-way ANOVA. *P < 0.05; **P < 0.01; NS, No significant difference.