| Abstract | Beyond the well‐defined role of the Eph (eryt�����hropoietin‐producing hepatocellular) receptor tyrosine kinases in developmental processes, cell motility, cell trafficking/adhesion, and cancer, nothing is known about their involvement in liver pathologies. During blood‐stage rodent malaria infection we have found that EphB2 transcripts and protein�������s were up‐regulated in the liver, a result likely driven by elevated surface expression on immune cells including macrophages. This was significant for malaria pathogenesis because EphB2–/– mice were protected from malaria‐induced liver fibrosis despite having a similar liver parasite burden compared with litterm�������ate control mice. This p�����rotection was correlated with a defect in the inflammatory potential of hepatocytes from EphB2–/– mice resulting in a reduction in adhesion molecules, chemokine/chemokine receptor RNA levels, and infiltration of leukocytes including macrophages/Kupffer cells, which mediate liver fibrosis during rodent malaria infections. These observations are recapitulated in the we�����ll‐established carbon tetrachloride model of liv������er fibrosis in which EphB2–/– carbon tetrachloride–treated mice showed a significant reduction of liver fibrosis compared to carbon tetrachloride–treated littermate mice. Depletion of macrophages by clodronate‐liposomes abrogates liver ������;EphB2 messenger RNA and protein up‐regulation and fibrosis in malaria‐infected���� mice. Conclusion: During rodent malaria, EphB2 expressio������n promotes malaria‐associated liver fibrosis; to our knowledge, our data are the first to implicate the EphB family of receptor tyrosine kinases in liver fibrosis or in the pathogenesis of malaria infection. |
