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Long trimer-immunization interval and appropriate adjuvant reduce immune responses to the soluble HIV-1-envelope trimer base

Authors :
Duan, H
Corrigan, AR
Cheng, C
Biju, A
Gonelli, CA
Olia, AS
Teng, I-T
Xu, K
O'Dell, S
Narpala, S
Castro, M
Serebryannyy, L
Wang, J
Parchment, DK
Sarfo, EK
van Schooten, J
Todd, J-P
Wang, S
Harris, DR
Geng, H
Jafari, AJ
Program, VRCP
Woodward, RA
Doria-Rose, NA
Foulds, KE
Mcdermott, AB
Gils, MJV
Koup, RA
Pierson, TC
Kwong, PD
Mascola, JR
Duan, H
Corrigan, AR
Cheng, C
Biju, A
Gonelli, CA
Olia, AS
Teng, I-T
Xu, K
O'Dell, S
Narpala, S
Castro, M
Serebryannyy, L
Wang, J
Parchment, DK
Sarfo, EK
van Schooten, J
Todd, J-P
Wang, S
Harris, DR
Geng, H
Jafari, AJ
Program, VRCP
Woodward, RA
Doria-Rose, NA
Foulds, KE
Mcdermott, AB
Gils, MJV
Koup, RA
Pierson, TC
Kwong, PD
Mascola, JR
Publication Year :
2024

Abstract

Soluble 'SOSIP'-stabilized HIV-1 envelope glycoprotein (Env) trimers elicit dominant antibody responses targeting their glycan-free base regions, potentially diminishing neutralizing responses. Previously, using a nonhuman primate model, we demonstrated that priming with fusion peptide (FP)-carrier conjugate immunogens followed by boosting with Env trimers reduced the anti-base response. Further, we demonstrated that longer immunization intervals further reduced anti-base responses and increased neutralization breadth. Here, we demonstrate that long trimer-boosting intervals, but not long FP immunization intervals, reduce the anti-base response. Additionally, we identify that FP priming before trimer immunization enhances antibody avidity to the Env trimer. We also establish that adjuvants Matrix M and Adjuplex further reduce anti-base responses and increase neutralizing titers. FP priming, long trimer-immunization interval, and an appropriate adjuvant can thus reduce anti-base antibody responses and improve Env-directed vaccine outcomes.

Details

Database :
OAIster
Publication Type :
Electronic Resource
Accession number :
edsoai.on1456027836
Document Type :
Electronic Resource