Human Vaccines & Immunotherapeutics (Dec 2017)

Screening of primary gp120 immunogens to formulate the next generation polyvalent DNA prime-protein boost HIV-1 vaccines

  • Shixia Wang,
  • Te-hui Chou,
  • Anthony Hackett,
  • Veronica Efros,
  • Yan Wang,
  • Dong Han,
  • Aaron Wallace,
  • Yuxin Chen,
  • Guangnan Hu,
  • Shuying Liu,
  • Paul Clapham,
  • James Arthos,
  • David Montefiori,
  • Shan Lu

DOI
https://doi.org/10.1080/21645515.2017.1380137
Journal volume & issue
Vol. 13, no. 12
pp. 2996 – 3009

Abstract

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Our previous preclinical studies and a Phase I clinical trial DP6-001 have indicated that a polyvalent Env formulation was able to elicit broadly reactive antibody responses including low titer neutralizing antibody responses against viral isolates of subtypes A, B, C and AE. In the current report, a panel of 62 gp120 immunogens were screened in a rabbit model to identify gp120 immunogens that can elicit improved binding and neutralizing antibody responses and some of them can be included in the next polyvalent formulation. Only about 19% of gp120 immunogens in this panel were able to elicit neutralizing antibodies against greater than 50% of the viruses included in a high throughput PhenoSense neutralization assay when these immuongens were tested as a DNA prime followed by a fixed 5-valent gp120 protein vaccine boost. The new polyvalent formulation, using five gp120 immunogens selected from this subgroup, elicited improved quality of antibody responses in rabbits than the previous DP6-001 formulation. More significantly, this new polyvalent formulation elicited higher antibody responses against a panel of gp70V1/V2 antigens expressing V1/V2 sequences from diverse subtypes. Bioinformatics analysis supports the design of a 4-valent or 5-valent formulation using gp120 immunogens from this screening study to achieve a broad coverage against 16 HIV-1 subtypes.

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