Inflammatory monocytes recruited to the liver within 24 hours after virus-induced inflammation resemble Kupffer cells but are functionally distinct.
Dowty MovitaMartijn D B van de GardePaula BiestaKim KreefftBart HaagmansElina ZunigaFlorence HerschkeSandra De JongheHarry L A JanssenLucio GamaAndre BoonstraThomas VanwolleghemPublished in: Journal of virology (2015)
Insights into how the immune system deals with hepatitis B virus (HBV) and HCV are scarce due to the lack of adequate animal model systems. This knowledge is, however, crucial to developing new antiviral strategies aimed at eradicating these chronic infections. We model virus-host interactions during the initial phase of liver inflammation 24 h after inoculating mice with LCMV. We show that infected Kupffer cells are rapidly outnumbered by infiltrating inflammatory monocytes, which secrete proinflammatory cytokines but are less phagocytic. Nevertheless, these recruited inflammatory monocytes start to resemble Kupffer cells on a transcript level. The specificity of these cellular changes for virus-induced liver inflammation is corroborated by demonstrating opposite functions of monocytes after LPS challenge. Overall, this demonstrates the enormous functional and genetic plasticity of infiltrating monocytes and identifies them as an important target cell for future treatment regimens.
Keyphrases
- oxidative stress
- hepatitis b virus
- induced apoptosis
- cell cycle arrest
- diabetic rats
- peripheral blood
- dendritic cells
- hepatitis c virus
- endoplasmic reticulum stress
- healthcare
- stem cells
- immune response
- gene expression
- signaling pathway
- cell death
- liver failure
- mesenchymal stem cells
- drug induced
- bone marrow
- cell therapy
- inflammatory response
- insulin resistance
- current status
- high fat diet induced