Author: Bleau, Christian; Burnette, Mélanie; Filliol, Aveline; Piquetâ€Pellorce, Claire; Samson, Michel; Lamontagne, Lucie
Title: Tollâ€like receptorâ€2 exacerbates murine acute viral hepatitis Cord-id: twkvk0vp Document date: 2016_8_10
ID: twkvk0vp
Snippet: Viral replication in the liver is generally detected by cellular endosomal Tollâ€like receptors (TLRs) and cytosolic helicase sensors that trigger antiviral inflammatory responses. Recent evidence suggests that surface TLR2 may also contribute to viral detection through recognition of viral coat proteins but its role in the outcome of acute viral infection remains elusive. In this study, we examined in vivo the role of TLR2 in acute infections induced by the highly hepatotrophic mouse hepatitis
Document: Viral replication in the liver is generally detected by cellular endosomal Tollâ€like receptors (TLRs) and cytosolic helicase sensors that trigger antiviral inflammatory responses. Recent evidence suggests that surface TLR2 may also contribute to viral detection through recognition of viral coat proteins but its role in the outcome of acute viral infection remains elusive. In this study, we examined in vivo the role of TLR2 in acute infections induced by the highly hepatotrophic mouse hepatitis virus (MHV) type 3 and weakly hepatotrophic MHVâ€A59 serotype. To address this, C57BL/6 (wildâ€type; WT) and TLR2 knockout (KO) groups of mice were intraperitoneally infected with MHV3 or MHVâ€A59. MHV3 infection provoked a fulminant hepatitis in WT mice, characterized by early mortality and high alanine and aspartate transaminase levels, histopathological lesions and viral replication whereas infection of TLR2 KO mice was markedly less severe. MHVâ€A59 provoked a comparable mild and subclinical hepatitis in WT and TLR2 KO mice. MHV3â€induced fulminant hepatitis in WT mice correlated with higher hepatic expression of interferonâ€Î², interleukinâ€6, tumour necrosis factorâ€Î±, CXCL1, CCL2, CXCL10 and alarmin (interleukinâ€33) than in MHVâ€A59â€infected WT mice and in MHV3â€infected TLR2 KO mice. Intrahepatic recruited neutrophils, natural killer cells, natural killer T cells or macrophages rapidly decreased in MHV3â€infected WT mice whereas they were sustained in MHVâ€A59â€infected WT mice and MHV3â€infected TLR2 KO. MHV3 in vitro infection of macrophagic cells induced rapid and higher viral replication and/or interleukinâ€6 induction in comparison to MHVâ€A59, and depended on viral activation of TLR2 and p38 mitogenâ€activated protein kinase. Taken together, these results support a new aggravating inflammatory role for TLR2 in MHV3â€induced acute fulminant hepatitis.
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