Protective efficacy of the anti-HIV broadly neutralizing antibody PGT121 in the context of semen exposure

BACKGROUND: HIV-1 infections occur following viral exposure at anogenital mucosal surfaces in the presence of semen. Semen contains immunosuppressive and pro-inflammatory factors. Semen from HIV-1-infected donors contains anti-HIV-1 antibodies. We assessed if passively infused anti-HIV-1 neutralizin...

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Detalles Bibliográficos
Autores principales: Parsons, Matthew S., Kristensen, Anne B., Selva, Kevin J., Lee, Wen Shi, Amarasena, Thakshila, Esterbauer, Robyn, Wheatley, Adam K., Bavinton, Benjamin R., Kelleher, Anthony D., Grulich, Andrew E., Khoury, Georges, Juno, Jennifer A., Kent, Stephen J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2021
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8361295/
https://www.ncbi.nlm.nih.gov/pubmed/34385004
http://dx.doi.org/10.1016/j.ebiom.2021.103518
Descripción
Sumario:BACKGROUND: HIV-1 infections occur following viral exposure at anogenital mucosal surfaces in the presence of semen. Semen contains immunosuppressive and pro-inflammatory factors. Semen from HIV-1-infected donors contains anti-HIV-1 antibodies. We assessed if passively infused anti-HIV-1 neutralizing antibody conferred protection from rectal SHIV(SF162P3) challenge at semen exposed mucosae. METHODS: We pooled seminal plasma from HIV-1-infected donors. The pool was screened by ELISA for antibodies against HIV-1(SF162) gp140. The ability of seminal plasma to inhibit macaque NK cells from responding to direct and antibody-dependent stimulation was assessed. The ability of seminal plasma to inhibit macaque granulocytes from mediating oxidative burst was also assessed. To demonstrate viral infectivity in the presence of seminal plasma, macaques (n = 4) were rectally challenged with SHIV(SF162P3) following exposure to 2.5 mL of seminal plasma. To evaluate if anti-HIV-1 neutralizing antibody confers protection against rectal SHIV challenge at semen exposed mucosae, eight macaques were intravenously infused with PGT121, either wild type (n = 4) or the Fc receptor binding deficient LALA variant (n = 4), and rectally challenged with SHIV(SF162P3) following exposure to 2.5 mL of seminal plasma. FINDINGS: Anti-HIV-1(SF162) gp140 antibodies were detected in seminal plasma. Seminal plasma inhibited direct and antibody-dependent NK cell activation and granulocyte oxidative burst in vitro. Rectal SHIV(SF162P3) challenge of control macaques following seminal plasma exposure resulted in infection of all animals. All macaques infused with wild type or LALA PGT121 and challenged with SHIV(SF162P3) following seminal plasma exposure were protected. INTERPRETATION: PGT121 conferred protection against rectal SHIV(SF162P3) challenge at semen exposed mucosae. Future research should investigate if semen alters protection conferred by antibodies more dependent on non-neutralizing functions.

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