AI Article Synopsis
- Researchers are aiming to create an effective HIV-1 vaccine that can produce strong and broadly neutralizing antibodies (bNAbs), but this goal is still unmet.
- The study tested various prime/boost vaccination regimens in guinea pigs over 200 weeks using different HIV-1 envelope proteins, finding that two tetravalent regimens outperformed a monovalent one in producing specific antibody responses.
- Despite increased responses to tier 1 neutralizing antibodies, the regimens did not enhance tier 2 neutralizing antibody responses, indicating that more innovative immunogen designs are needed to achieve widespread immunity against HIV-1.
Article Abstract
A vaccination regimen capable of eliciting potent and broadly neutralizing antibodies (bNAbs) remains an unachieved goal of the HIV-1 vaccine field. Here, we report the immunogenicity of longitudinal prime/boost vaccination regimens with a panel of HIV-1 envelope (Env) gp140 protein immunogens over a period of 200 weeks in guinea pigs. We assessed vaccine regimens that included a monovalent clade C gp140 (C97ZA012 [C97]), a tetravalent regimen consisting of four clade C gp140s (C97ZA012, 459C, 405C, and 939C [4C]), and a tetravalent regimen consisting of clade A, B, C, and mosaic gp140s (92UG037, PVO.4, C97ZA012, and Mosaic 3.1, respectively [ABCM]). We found that the 4C and ABCM prime/boost regimens were capable of eliciting greater magnitude and breadth of binding antibody responses targeting variable loop 2 (V2) over time than the monovalent C97-only regimen. The longitudinal boosting regimen conducted over more than 2 years increased the magnitude of certain tier 1 NAb responses but did not increase the magnitude or breadth of heterologous tier 2 NAb responses. These data suggest that additional immunogen design strategies are needed to induce broad, high-titer tier 2 NAb responses. The elicitation of potent, broadly neutralizing antibodies (bNAbs) remains an elusive goal for the HIV-1 vaccine field. In this study, we explored the use of a long-term vaccination regimen with different immunogens to determine if we could elicit bNAbs in guinea pigs. We found that longitudinal boosting over more than 2 years increased tier 1 NAb responses but did not increase the magnitude and breadth of tier 2 NAb responses. These data suggest that additional immunogen designs and vaccination strategies will be necessary to induce broad tier 2 NAb responses.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6002713 | PMC |
| http://dx.doi.org/10.1128/JVI.00369-18 | DOI Listing |
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