Hepatitis C, Chronic Clinical Trial
Official title:
Safety/Efficacy of Vaccination With Autologous Dendritic Cells Pulsed With Recombinant HCV-Antigens (Core and NS3) for Treatment of Patients With Chronic HCV-Infection
Clearance of HCV infection requires early and multi-specific HLA class I restricted CD8+ T
cell and class II restricted CD4+ T cell responses to both structural (Core) and
non-structural HCV proteins (NS3, NS4A, NS5A, NS5B). Dendritic cells (DCs) are professional
antigen-presenting cells that link innate and adaptive immune responses, and play a major
role in priming, initiating, and sustaining strong anti-HCV T cell immune responses.
The general objective of this study is to evaluate safety, feasibility and clinical efficacy
of therapeutic vaccination in genotype 1 HCV patients using autologous DCs pulsed with
recombinant HCV-antigens (Core and NS3). Expected effects: DC vaccination induces
Core/NS3-specific immune response and reduces viral load in patients with chronic
HCV-infection.
Hepatitis C virus (HCV) has chronically infected an estimated 170 million people worldwide.
People infected with HCV are at risk for developing chronic liver diseases, such as liver
cirrhosis and primary hepatocellular carcinoma. It has been estimated that HCV accounts for
27% of cirrhosis and 25% of hepatocellular carcinoma worldwide. Therapy for chronically
HCV-infected patients has involved a pegylated interferon-alpha and ribavirin (pegIFN/RBV)
and is still the only FDA-approved therapeutic combination. However, this therapy is
expensive, non-specific, toxic, and only effective in about 50% of genotype-1 HCV patients.
An early immune response, represented by the activation of NK cells, the development of
vigorous anti-HCV CD4+ and CD8+ T-cell responses, and the appearance of HCV-specific
antibodies, is mounted by the host during acute HCV infection and leads to clearance of the
virus. However, in the vast majority (≈85%) of infected individuals HCV causes a persistent
infection. The mechanisms of HCV persistence remain elusive and are largely related to
inefficient clearance of the virus by the host immune system.
Although HCV genome is very variable with hundreds of serotypes and six genotypes, several
structural (Core) and nonstructural proteins (NS3, NS4A, NS5A, NS5B) are highly conserved
among genotypes and subtypes. It is apparent that clearance of hepatitis C infection requires
early and multi-specific HLA class I restricted CD8+ T cell and class II restricted CD4+ T
cell responses to both structural and non-structural HCV proteins.
DCs are professional antigen-presenting cells that link innate and adaptive immune responses.
DCs play a major role in priming, initiating, and sustaining strong T cell responses against
pathogen-derived antigens. Therefore DC-based therapy represents a promising
immunotherapeutic approach in terms of their propensity to establish anti-HCV adaptive immune
responses.
This trial is a prospective, non-blinded, interventional study to determine safety,
feasibility and clinical efficacy of therapeutic vaccination in genotype 1 HCV patients using
autologous DCs pulsed with recombinant HCV-antigens (Core and NS3). Our previous work has
shown that the short-term loading of DCs with recombinant HCV proteins Core (1-120) and NS3
(1192-1457) have no any marked inhibitory effect on maturation and functions of DCs.
In experimental group thirty patients with chronic hepatitis C (genotype 1) will be
vaccinated via intracutaneous injection of monocyte-derived DCs, generated in the presence of
IFN-α/GM-CSF and pulsed with recombinant HCV Core (1-120) and NS3 (1192-1457) proteins. The
vaccination protocol will includes initiating (one injection per week, no 4) and maintaining
(one injection per month, no 6) courses with subsequent 6-month of follow up.
The safety will be determined by the evaluation of the number of participants with the
adverse events. Liver safety will be assessed by blood analysis and Ultrasound. Patients will
be monitored in a 2 months (after completing of initiating course), 7 months (after
completing of maintaining course) and 13 months (in a 6 months post-vaccination follow-up).
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