Recent studies have reported that founder viruses play unique roles in establishing HIV-1 infection. Understanding the biological and immunological features of envelope glycoproteins (Env) from such viruses may facilitate the development of effective vaccines against HIV-1. In this report, we evaluated the immunogenicity of gp120 immunogens from two pairs of clade B and two pairs of clade C mother-to-child transmitted (MTCT) HIV-1 variants that had various levels of sensitivity to broadly neutralizing monoclonal antibodies. Individual gp120 DNA and protein vaccines were produced from each of the eight MTCT Env antigens included in the current study. Rabbits were immunized with these gp120 immunogens by the DNA prime-protein boost approach. High level Env-specific antibody responses were elicited by all MTCT gp120 immunogens. However, their abilities to elicit neutralizing antibody (NAb) responses differed and those from relatively neutralization-resistant variants tended to be more effective in eliciting broader NAb. Results of this pilot study indicated that not all MTCT Env proteins have the same potential to elicit NAb. Understanding the mechanism(s) behind such variation may provide useful information in formulating the next generation of HIV vaccines.
Pilot study on the immunogenicity of paired Env immunogens from mother-to-child transmitted HIV-1 isolates.
对母婴传播的 HIV-1 分离株的配对 Env 免疫原的免疫原性进行初步研究
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作者:Wang Shixia, Kishko Michael, Wan Shengqin, Wang Yan, Brewster Frank, Gray Glenda E, Violari Avye, Sullivan John L, Somasundaran Mohan, Luzuriaga Katherine, Lu Shan
| 期刊: | Human Vaccines & Immunotherapeutics | 影响因子: | 3.500 |
| 时间: | 2012 | 起止号: | 2012 Nov 1; 8(11):1638-47 |
| doi: | 10.4161/hv.22414 | 研究方向: | 免疫/内分泌 |
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