CXCR6+CD69+ CD8+ T cells in ascites are associated with disease severity in patients with cirrhosis
Christian Niehaus, Sebastian Klein, Benedikt Strunz, Erich Freyer, Benjamin Maasoumy, Heiner Wedemeyer, Niklas K. Björkström, Anke Kraft, Markus Cornberg
Abstract
Background & AimsPatients with advanced liver cirrhosis often develop hepatic decompensation, which is accompanied by systemic inflammation and may eventually lead to acute-on-chronic liver failure (ACLF). One important cause of systemic hyperinflammation is a dysregulated overshooting immune response in ascites in the abdominal cavity. In this study we analyzed the role of CD8+ T cells in the ascites immune compartment.MethodsPeripheral blood and ascites fluid were collected from 50 patients with decompensated cirrhosis. Phenotype and functional responses of CD8+ T cells were analyzed and obtained data were compared to each other as well as to healthy controls and compensated cirrhosis patients.ResultsHigh-dimensional flow cytometry revealed that CD8+ T cells are abundant in the ascites of patients with liver cirrhosis and exhibit a chronically activated bystander phenotype with innate-like functions. Indeed, we identified distinct CXCR6+CD69+ clusters of late effector-memory CD8+ T cells that were rarely found in blood and correlated with clinical parameters of disease severity. Moreover, this CD8+ T cell population was hyperresponsive to innate cytokines and exhibited cytokine-mediated bystander activation. Interestingly, the Janus kinase (JAK) inhibitor tofacitinib was able to effectively block bystander-activated CXCR6+CD69+CD8+ T cells and significantly suppress effector molecule production.ConclusionsThese results indicate that CXCR6+CD69+ CD8+ T cells in ascites are associated with disease severity and may contribute to inflammation in patients with decompensated liver cirrhosis, suggesting that targeted inhibition of this immune cell subset may be a viable therapeutic option.Impact and implicationsPatients with advanced liver cirrhosis often develop hepatic decompensation, which is accompanied by systemic inflammation and eventually lead to acute-on-chronic liver failure (ACLF). One important cause of systemic hyperinflammation is a dysregulated overshooting immune response in ascites in the abdominal cavity. Here, we demonstrate that CXCR6+CD69+ CD8+ T cells are abundant in the ascites of patients with liver cirrhosis, exhibit a chronically activated bystander phenotype, and correlate with clinical parameters of disease severity. Moreover, we show that the Janus kinase (JAK) inhibitor tofacitinib is able to effectively block these bystander-activated CXCR6+CD69+ CD8+ T cells, suggesting that targeted inhibition of this immune cell subset may be a potential therapeutic strategy.Clinical trial numberProspective registry: INFEKTA (DRKS00010664)