4.6 Article

Live Simian Immunodeficiency Virus Vaccine Correlate of Protection: Immune Complex-Inhibitory Fc Receptor Interactions That Reduce Target Cell Availability

Journal

JOURNAL OF IMMUNOLOGY
Volume 193, Issue 6, Pages 3126-3133

Publisher

AMER ASSOC IMMUNOLOGISTS
DOI: 10.4049/jimmunol.1400822

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Funding

  1. National Institutes of Health [AI071306, RR00168]
  2. National Cancer Institute, National Institutes of Health [HHSN261200800001E]
  3. International AIDS Vaccine Initiative

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Principles to guide design of an effective vaccine against HIV are greatly needed, particularly to protect women in the pandemic's epicenter in Africa. We have been seeking these principles by identifying correlates of the robust protection associated with SIVmac239 Delta nef vaccination in the SIV-rhesus macaque animal model of HIV-1 transmission to women. We identified one correlate of SIVmac239 Delta nef protection against vaginal challenge as a resident mucosal system for SIV-gp41 trimer Ab production and neonatal FcR-mediated concentration of these Abs on the path of virus entry to inhibit establishment of infected founder populations at the portal of entry. In this study, we identify blocking CD4(+) T cell recruitment to thereby inhibit local expansion of infected founder populations as a second correlate of protection. Virus-specific immune complex interactions with the inhibitory Fc gamma RIIb receptor in the epithelium lining the cervix initiate expression of genes that block recruitment of target cells to fuel local expansion. Immune complex-Fc gamma RIIb receptor interactions at mucosal frontlines to dampen the innate immune response to vaginal challenge could be a potentially general mechanism for the mucosal immune system to sense and modulate the response to a previously encountered pathogen. Designing vaccines to provide protection without eliciting these transmission-promoting innate responses could contribute to developing an effective HIV-1 vaccine.

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