Table 1.
Recombinant protein hepatitis C vaccine studies.
| Structure (Investigator) | Phase (year) |
Subjects | Outcome | Ref. |
|---|---|---|---|---|
| HCV E1 + alum adjuvant (Innogenetics/GenImmune) |
I (2003) | 20 healthy volunteers + 34 HCV-infected, treatment- naive patients |
Well tolerated. No HCV viral load change. 50 out of 54 patient T-cell response. Humoral response correlated with improvement in ALT and liver histology |
[77,78] |
| II (2008) | 122 HCV-infected patients randomized (3:1) |
Well tolerated. Induced humoral and cellular immune responses. No change in histological progression of liver disease over 3 years |
[79] | |
| HCV E1/E2 glycoproteins/ MF59C adjuvant (Novartis) |
I (2010) | 60 healthy volunteers | Well tolerated. Induced antibody and E1/E2-specific T-cell responses in all patients independent of vaccine dose |
[76] |
| GI5005: recombinant yeast transfected with HCV NS3–core fusion protein (Globeimmune) |
II (2009) | 66 patients with chronic HCV-G1 (treatment-naive and nonresponders) |
17% SVR with vaccine + standard care, compared with standard therapy response of 5% in prior nonresponders |
[80] |
| HCV core protein/ISCOMATRIX® (CSL Ltd) |
I/IIa (2009) | 30 healthy volunteers | Well tolerated, mild local redness; all developed antibody response |
[82] |
Recombinant protein hepatitis C vaccine advantages: well tolerated with low toxicity; induces cross-neutralizing antibodies; proof-of-concept (HBV vaccine).
Disadvantages: generally only weak T-cell responses elicited.
ALT: Alanine transaminase; HCV: Hepatitis C virus; SVR: Sustained virological response.