Novel Adenovirus-Based Vaccines Induce Broad and Sustained T Cell Responses to HCV in Man

被引:314
作者
Barnes, Eleanor [1 ,2 ]
Folgori, Antonella [3 ]
Capone, Stefania [3 ]
Swadling, Leo [1 ]
Aston, Stephen [1 ]
Kurioka, Ayako [1 ]
Meyer, Joel [1 ]
Huddart, Rachel [1 ]
Smith, Kira [1 ]
Townsend, Rachel [1 ]
Brown, Anthony [1 ]
Antrobus, Richard [1 ]
Ammendola, Virginia [3 ]
Naddeo, Mariarosaria [3 ]
O'Hara, Geraldine [1 ]
Willberg, Chris [1 ]
Harrison, Abby [1 ]
Grazioli, Fabiana [4 ]
Esposito, Maria Luisa [4 ]
Siani, Loredana [3 ]
Traboni, Cinzia [3 ]
Oo, Ye [5 ]
Adams, David [5 ]
Hill, Adrian [1 ,2 ]
Colloca, Stefano [3 ]
Nicosia, Alfredo [3 ]
Cortese, Riccardo [3 ]
Klenerman, Paul [1 ,2 ]
机构
[1] Univ Oxford, Nuffield Dept Med, Oxford OX1 3SY, England
[2] John Radcliffe Hosp, Oxford NIHR Biomed Res Ctr, Oxford OX3 9DU, England
[3] Okairos, I-00040 Rome, Italy
[4] CEINGE, I-80145 Naples, Italy
[5] Univ Birmingham, NIHR Liver Biomed Res Unit, Birmingham B15 2TT, W Midlands, England
基金
英国惠康基金; 英国医学研究理事会;
关键词
C VIRUS-INFECTION; IMMUNE-RESPONSES; CD8(+); MEMORY; PERSISTENCE; EXPRESSION; PROTECTION; CLEARANCE;
D O I
10.1126/scitranslmed.3003155
中图分类号
Q2 [细胞生物学];
学科分类号
071013 [干细胞生物学];
摘要
Currently, no vaccine exists for hepatitis C virus (HCV), a major pathogen thought to infect 170 million people globally. Many studies suggest that host T cell responses are critical for spontaneous resolution of disease, and preclinical studies have indicated a requirement for T cells in protection against challenge. We aimed to elicit HCV-specific T cells with the potential for protection using a recombinant adenoviral vector strategy in a phase 1 study of healthy human volunteers. Two adenoviral vectors expressing NS proteins from HCV genotype 1B were constructed based on rare serotypes [human adenovirus 6 (Ad6) and chimpanzee adenovirus 3 (ChAd3)]. Both vectors primed T cell responses against HCV proteins; these T cell responses targeted multiple proteins and were capable of recognizing heterologous strains (genotypes 1A and 3A). HCV-specific T cells consisted of both CD4(+) and CD8(+) T cell subsets; secreted interleukin-2, interferon-gamma, and tumor necrosis factor-alpha; and could be sustained for at least a year after boosting with the heterologous adenoviral vector. Studies using major histocompatibility complex peptide tetramers revealed long-lived central and effector memory pools that retained polyfunctionality and proliferative capacity. These data indicate that an adenoviral vector strategy can induce sustained T cell responses of a magnitude and quality associated with protective immunity and open the way for studies of prophylactic and therapeutic vaccines for HCV.
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