Germline-targeting SOSIP trimer immunization elicits precursor CD4 binding-site targeting broadly neutralizing antibodies in infant macaques

Author:

Nelson Ashley N.,Shen Xiaoying,Vekatayogi Sravani,Zhang Shiyu,Ozorowski Gabriel,Dennis Maria,Sewall Leigh M.,Milligan Emma,Davis Dominique,Cross Kaitlyn A.,Chen Yue,van Schooten Jelle,Eudailey Joshua,Isaac John,Memon Saad,Weinbaum Carolyn,Stanfield-Oakley Sherry,Byrd Alliyah,Chutkan Suni,Berendam Stella,Cronin Kenneth,Yasmeen Anila,Alam S. Munir,LaBranche Celia C.,Rogers Kenneth,Shirreff Lisa,Cupo Albert,Derking Ronald,Villinger Francois,Klasse Per Johan,Ferrari Guido,Williams Wilton B.,Hudgens Michael G.,Ward Andrew B.ORCID,Montefiori David C.,Van Rompay Koen K.A.,Wiehe Kevin,Moore John P.,Sanders Rogier W.,De Paris Kristina,Permar Sallie R.

Abstract

AbstractA vaccine that can achieve protective immunity prior to sexual debut is critical to prevent the estimated 410,000 new HIV infections that occur yearly in adolescents. As children living with HIV can make broadly neutralizing antibody (bnAb) responses in plasma at a faster rate than adults, early childhood is an opportune window for implementation of a multi-dose HIV immunization strategy to elicit protective immunity prior to adolescence. Therefore, the goal of our study was to assess the ability of a B cell lineage-designed HIV envelope SOSIP to induce bnAbs in early life. Infant rhesus macaques (RMs) received either BG505 SOSIP or the germline-targeting BG505 GT1.1 SOSIP (n=5/group) with the 3M-052-SE adjuvant at 0, 6, and 12 weeks of age. All infant RMs were then boosted with the BG505 SOSIP at weeks 26, 52 and 78, mimicking a pediatric immunization schedule of multiple vaccine boosts within the first two years of life. Both immunization strategies induced durable, high magnitude binding antibodies and plasma autologous virus neutralization that primarily targeted the CD4-binding site (CD4bs) or C3/465 epitope. Notably, three BG505 GT1.1-immunized infants exhibited a plasma HIV neutralization signature reflective of VRC01-like CD4bs bnAb precursor development and heterologous virus neutralization. Finally, infant RMs developed precursor bnAb responses at a similar frequency to that of adult RMs receiving a similar immunization strategy. Thus, a multi-dose immunization regimen with bnAb lineage designed SOSIPs is a promising strategy for inducing protective HIV bnAb responses in childhood prior to adolescence when sexual HIV exposure risk begins.

Publisher

Cold Spring Harbor Laboratory

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