Study of a New MVA Vaccine for Hepatitis C Virus

Sponsor

ReiThera Srl (Industry)

Overall Status

Completed

CT.gov ID

NCT01296451

Collaborator

University of Oxford (Other), Oxford University Hospitals NHS Trust (Other), University Hospital Birmingham (Other)

Enrollment

Locations

Arms

Duration (Months)

18.3

Patients Per Site

0.3

Patients Per Site Per Month

Study Details

Study Description

Brief Summary

The study is aimed at assessing the safety of AdCh3NSmut and the new candidate vaccine MVA-NSmut when administered sequentially, or alone, to healthy volunteers and patients with hepatitis C virus infection The study also aims at assessing the cellular immune response generated by AdCh3NSmut and MVA-NSmut administered as mentioned above.

Condition or Disease	Intervention/Treatment	Phase
Hepatitis C Infection	Biological: MVA-NSmut Biological: AdCh3NSmut Biological: AdCh3NSmut1	Phase 1

Detailed Description

The scientific rationale supporting this study can be summarised as follows: an effective antiviral T cell response can mediate HCV viral control and induce the spontaneous resolution of HCV during primary infection. This observation strongly supports the case for the development of T cell induction strategies as a potential therapy for HCV. A hallmark of persistent HCV infection, when viral loads are high, is a weak and narrowly focused HCV specific T cell response, whereas in resolved infection with undetectable viral loads robust T cell responses are detected. Furthermore, mouse and other human models of persistent viral infection show that antigen load crucially determines the quality and quantity of the anti-viral T cell responses so generated [17-18]. This supports the case for the assessment of efficacy of T cell induction, a) in the setting of low viral loads following viral suppression with combination therapy, and b) in the setting of high viral loads. Since pre-existing anti-vector immunity to adenoviral vectors may limit vaccine efficacy, we have conducted a phase-I clinical trial in healthy human subjects using human (Ad6) and simian (AdCh3) adenoviral vectors found at low sero-prevalence in human populations, in a heterologous prime/boost regimen (study HCV001). The same vectors are also under investigation in HCV infected patients (HCV002). These vectors encode the HCV non-structural proteins with a genetically inactivated polymerase gene (NSmut). We have shown that both vectors are safe and highly immunogenic. In preclinical primate studies using identical vectors, heterologous boosting increased peak responses and long-term immunity. However, in humans it appears that, although HCV specific T-cell responses increase following boosting, the magnitude of this response is reduced compared to that observed during vaccine priming. This is probably due to the induction of cross-reactive immunity between the two vectors. In contrast, it has recently been shown that Modified Vaccinia Ankara (MVA) encoding the malaria antigen ME-TRAP very successfully boosts T-cell responses primed with a simian Adenovirus vector, inducing the highest level of CD4+ and CD8+ T-cell responses ever observed using a vectored vaccine and affording protection from malaria infection (A. Hill unpublished data).

For these reasons we now wish to assess an MVA construct encoding HCV NS that will be combined with AdCh3NSmut (or AdCh3NSmut1) in a heterologous prime/boost vaccination regimen to assess the safety and immunogenicity of this strategy in healthy and HCV infected patients. This study will address the following questions: In healthy volunteers:

Can vaccination with MVA-NSmut vector alone safely induce HCV specific T cell responses?
Can vaccination using a heterologous prime/boost vaccination schedule with AdCh3NSmut and MVA-NSmut safely induce HCV specific T cell responses?

In HCV infected patients can a heterologous prime/boost vaccination schedule using

AdCh3NSmut and MVA-NSmut:

Safely induce HCV specific T cell responses during pegylated-interferon and ribavirin (combination) therapy for HCV genotype-1 infection, after a significant decline in viral load, 14 weeks into therapy?
Safely induce HCV specific T cell responses during combination therapy for HCV genotype-1 infection, 2 weeks into therapy?
Safely induce HCV specific T cell responses in patients with chronic HCV (not receiving combination therapy) and a high viral load?
Suppress viral load in patients with chronic HCV, not on treatment with IFN and Ribavirin? Since the effect of combination therapy on HCV specific T cells is currently debated (see below) we will compare the T cell responses generated by the therapeutic prime/boost vaccination schedule in this study, to a group of matched historical control patients treated with combination therapy in whom immunological assessment has been made in an identical way to that proposed in this study.

Study Design

Study Type:

Interventional

Actual Enrollment :

55 participants

Allocation:

Non-Randomized

Intervention Model:

Parallel Assignment

Masking:

None (Open Label)

Primary Purpose:

Treatment

Official Title:

A Phase I Study to Assess the Safety and Immunogenicity of AdCh3NSmut and MVA-NSmut in Healthy Volunteers and Patients With Hepatitis C Virus Infection

Study Start Date :

Dec 1, 2010

Actual Primary Completion Date :

Jan 1, 2016

Actual Study Completion Date :

Jan 1, 2016

Arms and Interventions

Arm	Intervention/Treatment
Experimental: Arm A, group1 Intervention: MVA-NSmut. Administration schedule: 1 dose MVA-NSmut 2 x 10^8 pfu. Subjects: 4 healthy volunteers	Biological: MVA-NSmut Genetic vaccine against Hepatitis C virus infection
Experimental: Arm A, group 2 Interventions: AdCh3NSmut; MVA-NSmut. Administration schedule: 1 dose AdCh3NSmut 2.5 x 10^10vp at week 0 and 1 dose MVA-NSmut 2 x 10^8 pfu at week 8. Subjects: 10 healthy volunteers	Biological: MVA-NSmut Genetic vaccine against Hepatitis C virus infection Biological: AdCh3NSmut genetic vaccine against Hepatitis virus infection
Experimental: Arm B, group 1 Interventions: AdCh3NSmut; MVA-NSmut. Administration schedule: 1 dose AdCh3NSmut 2.5 x 10^10vp at week 14 and 1 dose MVA-NSmut 2 x 10^8pfu at week 22, after starting PEG-IFN and ribavirin therapy. Subjects: 5 patients	Biological: MVA-NSmut Genetic vaccine against Hepatitis C virus infection Biological: AdCh3NSmut genetic vaccine against Hepatitis virus infection
Experimental: Arm B, group 2 Interventions: AdCh3NSmut; MVA-NSmut.. Administration schedule: 1 dose AdCh3NSmut 2.5 x 1010vp at week 2 and 1 dose MVA-NSmut 2 x 108pfu at week 10, after starting PEG-IFN and ribavirin therapy. Subjects: 5 patients	Biological: MVA-NSmut Genetic vaccine against Hepatitis C virus infection Biological: AdCh3NSmut genetic vaccine against Hepatitis virus infection
Experimental: Arm C, group 1 Interventions: AdCh3NSmut; MVA-NSmut Administration schedule: 1 dose AdCh3NSmut 2.5 x 10^10vp at week 0 and 1 dose MVA-NSmut 2 x 10^8pfu at week 8. Subjects: 4 patients	Biological: MVA-NSmut Genetic vaccine against Hepatitis C virus infection Biological: AdCh3NSmut genetic vaccine against Hepatitis virus infection
Experimental: Arm A, group 3 Interventions: AdCh3NSmut; MVA-NSmut Administration schedule: 1 dose AdCh3NSmut 2.5 x 10^10vp at week 0, 1 dose MVA-NSmut 2 x 10^8pfu at week 8, 1 dose AdCh3NSmut 2.5 x 10^10vp at week 16 and 1 dose MVA-NSmut 2 x 10^8 pfu at week 24. Subjects: 5 healthy volunteers	Biological: MVA-NSmut Genetic vaccine against Hepatitis C virus infection Biological: AdCh3NSmut genetic vaccine against Hepatitis virus infection
Experimental: Arm A, group 4 Intervention: AdCh3NSmut; MVA-NSmut. Administration schedule: 1 dose AdCh3NSmut 2.5 x 10^10vp (at least 6 months after they were initially enrolled) and 1 dose MVA-NSmut 2 x 10^8 pfu 8 weeks later. Subjects: up to 5 healthy volunteers who were previously in group A2	Biological: MVA-NSmut Genetic vaccine against Hepatitis C virus infection Biological: AdCh3NSmut genetic vaccine against Hepatitis virus infection
Experimental: Experimental: Arm A, group5 Intervention: AdCh3NSmut1. MVA-NSmut. Administration schedule:1 dose AdCh3NSmut1 2.5 x 10^10vp at week 0, 1 dose MVA-NSmut 2 x 10^8 pfu at week 8 and 1 dose MVA-NSmut 2 x 10^8 pfu at week 40. Subjects: 5 healthy volunteers	Biological: MVA-NSmut Genetic vaccine against Hepatitis C virus infection Biological: AdCh3NSmut1 genetic vaccine against Hepatitis virus infection
Experimental: Arm A, group 6 Interventions: AdCh3NSmut1. Administration schedule: 1 dose AdCh3NSmut1 2.5 x 10^10 vp at week 0 and 1 dose MVA-NSmut 2 x 10^7 pfu at week 8. Subjects: 5 healthy volunteers	Biological: AdCh3NSmut1 genetic vaccine against Hepatitis virus infection
Experimental: Arm A, group 7 Interventions: AdCh3NSmut1; MVA-NSmut. Administration schedule: 1 dose AdCh3NSmut1 2.5 x 10^10 vp at week 0 and 1 dose MVA-NSmut 2 x 10^6 pfu at week 8. Subjects: 5 healthy volunteers	Biological: MVA-NSmut Genetic vaccine against Hepatitis C virus infection Biological: AdCh3NSmut1 genetic vaccine against Hepatitis virus infection

Outcome Measures

Primary Outcome Measures

Number of participant with adverse events, type and severity of adverse events [Different time frames depending on study groups]
To assess the safety of new hepatitis C vaccine candidates, AdCh3NSmut (and the improved version AdCh3NSmut1) and MVA-NSmut when administered to healthy volunteers and to HCV infected patients. The specific endpoints for safety will be actively collected data on adverse events.

Secondary Outcome Measures

Immunogenicity [Different time frames depending on the study groups]
To assess the cellular immune response generated by AdCh3NSmut (and the improved version AdCh3NSmut1) and MVA-NSmut, when administered sequentially, to patients with hepatitis C virus infection. The specific endpoint of cellular immune response will be collected via IFN-gamma ELISpot assay and other exploratory immunological tests.

Eligibility Criteria

Criteria

Ages Eligible for Study:

18 Years to 64 Years

Sexes Eligible for Study:

All

Accepts Healthy Volunteers:

Yes

Inclusion Criteria:

The healthy volunteers must satisfy all the following inclusion criteria to be eligible for the study (group A1 or A2):

Healthy adults aged 18 to 55 years (inclusive)
Resident in or near the trial sites for the duration of the vaccination study
Able and willing (in the Investigator's opinion) to comply with all study requirements
For women of child bearing potential, willingness to practice continuous effective contraception during the study and a negative pregnancy test on the day(s) of vaccination
Men, including those with pregnant partners, should use barrier contraception until 3 months after the last vaccination
Written informed consent

The patients with HCV in Groups B1, B2 and C1 must satisfy all the following inclusion criteria to be eligible for the study:

HCV infected with genotype-1 infection (any viral load)
Patients must not be currently receiving any treatment for HCV infection.
Adults aged 18 to 64 years (inclusive)
Resident in or near the trial sites for the duration of the vaccination study
Able and willing (in the Investigator's opinion) to comply with all study requirements
Liver transaminases may be within normal limits or elevated.
For men in Arm B, including those with pregnant partners, a willingness to use barrier contraception until six months after completing treatment with IFN/ribavirin
For women in Arm B, of child bearing potential, a willingness to practice continuous effective contraception during the study and a negative pregnancy test on the day(s) of vaccination.
For men in arm C, including those with pregnant partners, a willingness to use barrier contraception until three months after the last vaccination
Written informed consent
Patients with HCV in groups B1 and B2 must be treatment naïve to previous IFN and ribavirin combination therapy. They may be included if they have been previously treated with interferon monotherapy but relapsed after treatment.
Patients with HCV in groups C1 may be treatment naïve, or have been previously treated with interferon monotherapy or interferon and ribavirin therapy and relapsed after treatment

Exclusion Criteria:

The subjects (both healthy individuals or patients) may not enter the study if any of the following exclusion criteria apply:

Participation in another research study involving an investigational product in the 30 days preceding enrolment, or planned use during the study period
Prior receipt of a recombinant simian or human adenoviral vaccine
Clinical, biochemical (abnormal liver synthetic dysfunction defined by an elevated blood prothrombin time or a low blood albumin level), ultrasonographic, or liver biopsy (histology) evidence of cirrhosis or portal hypertension
Any confirmed or suspected immunosuppressive or immunodeficient state, including HIV infection; asplenia; recurrent, severe infections and chronic (more than 14 days) immunosuppressant medication within the past 6 months (inhaled and topical steroids are allowed)
History of allergic disease or reactions likely to be exacerbated by any component of the vaccine, e.g., Kathon
History of clinically significant contact dermatitis
Any history of anaphylaxis in reaction to vaccination
Pregnancy, lactation or willingness/intention to become pregnant during the study
History of cancer (except basal cell carcinoma of the skin and cervical carcinoma in situ)
Suspected or known current alcohol abuse as defined by an alcohol intake of greater than 42 units every week
Current suspected or known injecting drug abuse
Seropositive for hepatitis B surface antigen (HBsAg)
Seropositive for HIV (antibodies to HIV) at screening
Any other significant disease, disorder or finding, which, in the opinion of the Investigator, may either put the patient at risk because of participation in the study, or may influence the result of the study, or the patient's ability to participate in the study
Any other finding which in the opinion of the investigators would significantly increase the risk of having an adverse outcome from participating in the protocol
Individuals who have had a temperature >38°C in the 3 days preceding vaccination.
Patients likely to have been infected with HCV within the last 12 months

In addition to the above listed exclusion criteria:

Patients with HCV may not enter arms B1 and B2 of the study if any of the following exclusion criteria applies:

Patients are non-responders to previous IFN-alpha monotherapy
Patients who received IFN-alpha and ribavirin or PEG-IFN and ribavirin in the past and who were non-responders or who relapsed during or after therapy
Patients with a known allergy to ribavirin or interferon-alpha
Haemoglobin less than 10g/dl
Severe neutropenia or thrombocytopenia
Patients who have had a heart attack or who have suffered from any other severe heart disease in the last 6 months
Patients with haemoglobinopathies
Autoimmune hepatitis
Autoimmune disease
History of organ transplantation
Uncontrolled seizures
Uncontrolled severe psychiatric conditions

Patients with HCV may not enter arm C if they were previous non-responders to interferon monotherapy, or interferon and ribavirin combination therapy.

Contacts and Locations

Locations

	Site	City	State	Country	Postal Code
1	Centre for Clinical Vaccinology and Tropical Medicine	Oxford	Oxfordshire	United Kingdom	OX3 7LJ
2	John Radcliffe Hospital, Headley Way	Headington, Oxford		United Kingdom	OX3 9DU
3	Wycombe Hospital, High Wycombe, Buckinghamshire	High Wycombe		United Kingdom

Sponsors and Collaborators

ReiThera Srl
University of Oxford
Oxford University Hospitals NHS Trust
University Hospital Birmingham

Investigators

Study Chair: Eleanor Barnes, Dr., University of Oxford, UK
Principal Investigator: Paul Klenerman, Prof., University of Oxford, UK
Principal Investigator: David Gorard, Dr, Wycombe Hospital, High Wycombe, Buckinghamshire