4.7 Article

The Novel Replication-defective Vaccinia Virus (Tiantan Strain)-based Hepatitis C Virus Vaccine Induces Robust Immunity in Macaques

Journal

MOLECULAR THERAPY
Volume 21, Issue 9, Pages 1787-1795

Publisher

CELL PRESS
DOI: 10.1038/mt.2013.122

Keywords

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Funding

  1. 863 Hi-Tech Research and Development Program of China [2007AA02Z455]
  2. National Mega-project for Infectious Diseases of China [2013ZX10004-601, 2009ZX10004-705, 2009ZX10004-715]

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The induction of a robust neutralizing antibody (nAb) response is likely to be as essential as specific cell-mediated immunity (CMI) against multiple antigens for the development of effective preventive and therapeutic vaccines against hepatitis C virus (HCV) infection in humans. To date, no data on the imnnunogenicity of the replication-defective vaccinia virus (derived from the Tiantan strain) (rNTV)-based HCV vaccine in primates have been reported. This study describes in detail the immunogenicity of various vaccine candidates in rhesus macaques, including rNTV-based and replication-defective recombinant adenoviral (rAd)-based HCV vaccines, as well as HCV pseudotyped virus-like particles (HCVpp). Our data showed that rAd-HCV vaccine boosting induced robust CMI, while priming or boosting with HCVpp enhanced the antigen-specific nAb response after rAd-HCV vaccination; however, CMI was not enhanced. Vaccination includes rNTV-HCV priming induced robust antigen-specific antibody, particularly nAbs, and CM! responses. Furthermore, more robust and longer-lasting CMI and higher cytokine levels (both Th1 and Th2 types, especially IFN-gamma) resulted from boosting with rAd-HCV. We conclude that the rNTV-based HCV vaccine induces robust nAbs and CMI when combined with a heterogeneous primer-booster strategy, which shows promise for development of a human HCV vaccine.

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