Chronic Hepatitis C Infection Clinical Trial
Official title:
The Role of FGL2-FcgammaRIIB Inhibitory Pathway in Human Viral Hepatitis
Viral hepatitis is a serious world health problem affecting over 1 billion people worldwide. Presently the lack of highly effective treatments results in many patients requiring liver transplantation or death. The investigators have defined the role of a unique molecule FGL2 and its receptor fc-gammaR and its role in the pathogenesis of both experimental and human hepatitis. The studies proposed in the present proposal will test the hypothesis that measuring levels of fgl2 in plasma will identify individuals that will go on to develop chronic disease and inhibition of binding of fgl2 to its receptor will allow the host with both acute and chronic disease to develop an appropriate immune response and clear the virus. The studies will provide rationale for generation of new therapies to improve the treatment of patients with acute and chronic viral hepatitis by targeting fgl2.
Hepatitis C Virus (HCV) infection affects more than 200 million individuals worldwide. Only
a fraction of infected individuals clear the virus, whereas the majority (70%) develops
chronic infection. The current standard of care, pegylated interferon/ ribavirin
(pegIFN/rib) is effective in only 50% of patients. Patients who fail anti-viral therapy
gradually progress to end-stage liver disease and hepatocellular cancer; which can only be
cured by a liver transplant. The reasons for treatment failure are unclear but involve both
viral and host factors. One significant factor may be impaired T cell function. Chronic HCV
infection is associated with functionally impaired or exhausted cytotoxic T lymphocytes
(CTLs), with decreased anti-viral cytokine production, cytotoxicity and proliferative
capacity. The investigators recently showed that many patients who fail treatment have
elevated frequencies of CD4+CD25+Foxp3+regulatory T cells (Tregs) producing the novel
fibrinogen-like-protein 2 (FGL2/fibroleukin) which appears to impair HCV specific immune
responses. Binding of FGL2 to the FcγRIIB receptor leads to inhibition of dendritic cell
(DC) maturation, B cell apoptosis and inhibition of development of effective CD4+and CD8+T
and B cell anti-viral responses. In HCV, increased levels of secreted FGL2 may suppress
anti-viral immune responses and promote disease progression.
Hypothesis: HCV suppresses innate and adaptive anti-viral immune responses through the
FGL2-FcγRIIB inhibitory pathway. Inhibition of this pathway will restore effective
virus-specific immunity and lead to successful viral eradication.
Significance: These studies will establish the importance of FGL2-FcγRIIB inhibitory pathway
in the pathogenesis of HCV chronic infection and provide a novel therapeutic approach to
improve virus eradication and long term patient outcomes.
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Observational Model: Case Control, Time Perspective: Prospective
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