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Guideview > News > Science News  > NIH's HIV Antibodies: Shielding Monkeys, Advancing Vaccine

NIH's HIV Antibodies: Shielding Monkeys, Advancing Vaccine

Discover how NIH-developed HIV antibodies protect monkeys from SHIV, a pivotal step in HIV vaccine research. Learn about promising fusion peptide-targeting antibodies. GuideView1 MIN READApril 28, 2024

In a significant stride towards the development of a preventive HIV vaccine, a recent proof-of-concept study demonstrates the efficacy of three distinct HIV antibodies in safeguarding monkeys from acquiring simian-HIV (SHIV). Published in Science Translational Medicine and led by the Vaccine Research Center (VRC) at the National Institute of Allergy and Infectious Diseases (NIAID), this study marks a pivotal step in HIV vaccine research.


Transmission electron micrograph of HIV-1 virus particles (red) budding and replicating from a segment of a chronically infected H9 cell (blue). Particles are in various stages of maturity; arc/semi-circles are immature particles that have started to form but are still part of the cell. Immature particles slowly change morphology into matNIAID Image Source: NIH Official Website



Key Findings


The antibodies utilized in the study include a human broadly neutralizing antibody, VRC34.01, and two antibodies isolated from previously vaccinated monkeys. These antibodies target the fusion peptide, a critical site on the HIV surface protein facilitating the virus's entry into cells. Notably, antibodies that target the fusion peptide have shown efficacy in neutralizing diverse strains of HIV in vitro.

Study Methodology

Rhesus macaques, commonly employed as an animal model for HIV vaccine research, received intravenous infusions of the antibodies or a placebo. Subsequently, they were challenged with a strain of SHIV. Remarkably, all monkeys in the placebo group acquired SHIV, whereas those administered with the antibodies exhibited varying degrees of protection.

Protective Efficacy

Monkeys receiving VRC34.01 infusions showed significant protection against SHIV acquisition. Moreover, the vaccine-elicited rhesus macaque antibodies, DFPH-a.15 and DF1W-a.01, also conferred considerable protection. However, the protective effect was dose-dependent, with higher antibody concentrations correlating with increased protection.

Implications and Future Directions

The study's findings underscore the potential of fusion peptide-directed antibodies in HIV vaccine development. The authors suggest further exploration of vaccine concepts targeting the fusion peptide, emphasizing the need to generate a diverse range of such antibodies to combat the extensive variability of HIV strains.


Conclusion

This groundbreaking research paves the way for the development of an effective HIV vaccine, offering hope in the fight against this global health challenge.

Highlights

  • Three HIV antibodies demonstrate efficacy in protecting monkeys from acquiring SHIV, a significant step towards an HIV vaccine.
  • Antibodies targeting the fusion peptide, a critical site on the HIV surface protein, exhibit promising neutralization capabilities against diverse HIV strains.
  • Monkeys administered with the antibodies show varying degrees of protection against SHIV acquisition, with higher antibody concentrations correlating with increased efficacy.
  • The study underscores the importance of further exploration into vaccine concepts targeting the fusion peptide, emphasizing the need for a diverse range of antibodies to combat HIV's extensive variability.
  NIH          
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