Author: Wu, Z. G.; Yan, W. M.; Guo, W.; Chen, T.; Zou, Y.; Wang, H. W.; Wang, X. J.; Yang, X. J.; Lu, Y. L.; Luo, X. P.; Ning, Q.
Title: Telbivudine preserves Tâ€helper 1 cytokine production and downregulates programmed death ligand 1 in a mouse model of viral hepatitis Cord-id: j9ld7q70 Document date: 2010_3_3
ID: j9ld7q70
Snippet: Summary. Telbivudine is an orally bioavailable Lâ€nucleoside with potent and specific antiâ€hepatitis B virus activity. The higher rate of hepatitis B e antigen (HBeAg) seroconversion during telbivudine treatment than other potent antiâ€HBV agents suggests a potential immunomodulatory effect. We sought to determine the effects of telbivudine on the immune system, particularly on cytokine production and Tâ€cell response, using an animal model with mouse hepatitis virus strain 3 (MHVâ€3)â€in
Document: Summary. Telbivudine is an orally bioavailable Lâ€nucleoside with potent and specific antiâ€hepatitis B virus activity. The higher rate of hepatitis B e antigen (HBeAg) seroconversion during telbivudine treatment than other potent antiâ€HBV agents suggests a potential immunomodulatory effect. We sought to determine the effects of telbivudine on the immune system, particularly on cytokine production and Tâ€cell response, using an animal model with mouse hepatitis virus strain 3 (MHVâ€3)â€induced hepatitis. The effects of telbivudine on virus replication and cytokine production were investigated in vitro using MHVâ€3â€infected macrophages, and the effects on Tâ€cell response were investigated in vivo in an MHVâ€3â€induced viral hepatitis model. Telbivudine had no effect on MHVâ€3 replication in macrophages. However, the production of tumour necrosis factorâ€Î± and interleukinâ€12 was increased significantly in MHVâ€3â€induced macrophages treated with telbivudine. In vivo survival was enhanced in telbivudineâ€treated mice, with marked normalization in clinical conditions and histological lesions. Serum levels of interferonâ€Î³ were elevated significantly after telbivudine treatment in MHVâ€3â€infected C3H mice. In contrast, serum interleukinâ€4 levels were decreased significantly. Furthermore, telbivudine treatment enhanced the ability of T cells to undergo proliferation and secrete cytokines but did not affect cytotoxicity of infected hepatocytes. Of note, we found that telbivudine treatment suppressed programmed death ligand 1 expression on T cells. The results demonstrate the immunomodulatory properties of telbivudine, independent of its antiviral activity, in a mouse model of MHVâ€3â€induced hepatitis.
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