T cell-inducing vaccine durably prevents mucosal SHIV infection even with lower neutralizing antibody titers

Author:

Arunachalam Prabhu S.,Charles Tysheena P.,Joag VineetORCID,Bollimpelli Venkata S.,Scott Madeleine K. D.,Wimmers Florian,Burton Samantha L.,Labranche Celia C.,Petitdemange Caroline,Gangadhara SailajaORCID,Styles Tiffany M.,Quarnstrom Clare F.,Walter Korey A.,Ketas Thomas J.,Legere Traci,Jagadeesh Reddy Pradeep Babu,Kasturi Sudhir Pai,Tsai Anthony,Yeung Bertrand Z.,Gupta Shakti,Tomai Mark,Vasilakos John,Shaw George M.,Kang Chil-Yong,Moore John P.ORCID,Subramaniam Shankar,Khatri Purvesh,Montefiori David,Kozlowski Pamela A.,Derdeyn Cynthia A.ORCID,Hunter EricORCID,Masopust DavidORCID,Amara Rama R.ORCID,Pulendran BaliORCID

Abstract

AbstractRecent efforts toward an HIV vaccine focus on inducing broadly neutralizing antibodies, but eliciting both neutralizing antibodies (nAbs) and cellular responses may be superior. Here, we immunized macaques with an HIV envelope trimer, either alone to induce nAbs, or together with a heterologous viral vector regimen to elicit nAbs and cellular immunity, including CD8+ tissue-resident memory T cells. After ten vaginal challenges with autologous virus, protection was observed in both vaccine groups at 53.3% and 66.7%, respectively. A nAb titer >300 was generally associated with protection but in the heterologous viral vector + nAb group, titers <300 were sufficient. In this group, protection was durable as the animals resisted six more challenges 5 months later. Antigen stimulation of T cells in ex vivo vaginal tissue cultures triggered antiviral responses in myeloid and CD4+ T cells. We propose that cellular immune responses reduce the threshold of nAbs required to confer superior and durable protection.

Funder

U.S. Department of Health & Human Services | National Institutes of Health

Bill and Melinda Gates Foundation

Publisher

Springer Science and Business Media LLC

Subject

General Biochemistry, Genetics and Molecular Biology,General Medicine

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