- 作者:Susanna Commandeura ; Susan J.F. van den Eedena ; Karin Dijkmana ; Simon O. Clarkc ; Krista E. van Meijgaardena ; Louis Wilsona ; Kees L.M.C. Frankena ; Ann Williamsc ; Dennis Christensenb ; Tom H.M. Ottenhoffa ; Annemieke Geluka ; a.geluk@lumc.nl" class="auth_mail
- 关键词:HLA-DR3 ; Infection-specific ; IVE-TB antigen ; Mtb ; Rv2034 ; TB vaccine
- 刊名:Vaccine
- 出版年:17 June 2014
- 年:2014
- 卷:32
- 期:29
- 页码:3580-3588
- 全文大小:1519 K
A minimal requirement for Mtb vaccine antigens is their in vivo expression during Mtb infection and ability to trigger significant immune responses. Recently we identified a new class of Mtb antigens, designated IVE-TB (in vivo expressed) antigens. These included Rv2034, a protein that was expressed during pulmonary infection and strongly recognized by human T-cells. Here, the in vivo immunogenicity and protective efficacy of Rv2034 was further analyzed using HLA-DR transgenic mice that lack endogenous murine MHC class II molecules. The Rv2034 protein indeed was highly immunogenic in HLA-DR3 transgenic mice and induced HLA-DR3 restricted IFN-纬+/TNF+ and IFN-纬+ CD4+ T-cells, specific for an epitope encoded in peptide 31–50. CD4+ T-cell responses were optimally induced when using TLR9- and TLR3-ligand-adjuvants or CAF09. Rv2034-specific antibodies were observed following immunization with either TLR2-, TLR3-, TLR4-, TLR5-, TLR7- or TLR9-ligands or CAF09. Importantly, immunization with Rv2034 or the hybrid-protein Ag85B-ESAT6-Rv2034 adjuvanted with CpG or CAF09, induced over one log reduction, relative to unvaccinated controls, in the number of bacilli in the lungs of Mtb challenged HLA-DR3 transgenic mice and guinea pigs. These data demonstrate the potential of Rv2034 as a novel, IVE-TB antigen for future TB vaccination.