Preexisting memory CD4+ T cells contribute to the primary response in an HIV-1 vaccine trial
Suzanne L. Campion, … , Persephone Borrow, Andrew J. McMichael
Suzanne L. Campion, … , Persephone Borrow, Andrew J. McMichael
Published December 1, 2021
Citation Information: J Clin Invest. 2021;131(23):e150823. https://doi.org/10.1172/JCI150823.
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Concise Communication Immunology

Preexisting memory CD4+ T cells contribute to the primary response in an HIV-1 vaccine trial

Abstract

Naive and memory CD4+ T cells reactive with human immunodeficiency virus type 1 (HIV-1) are detectable in unexposed, unimmunized individuals. The contribution of preexisting CD4+ T cells to a primary immune response was investigated in 20 HIV-1–seronegative volunteers vaccinated with an HIV-1 envelope (Env) plasmid DNA prime and recombinant modified vaccinia virus Ankara (MVA) boost in the HVTN 106 vaccine trial (clinicaltrials.gov NCT02296541). Prevaccination naive or memory CD4+ T cell responses directed against peptide epitopes in Env were identified in 14 individuals. After priming with DNA, 40% (8/20) of the elicited responses matched epitopes detected in the corresponding preimmunization memory repertoires, and clonotypes were shared before and after vaccination in 2 representative volunteers. In contrast, there were no shared epitope specificities between the preimmunization memory compartment and responses detected after boosting with recombinant MVA expressing a heterologous Env. Preexisting memory CD4+ T cells therefore shape the early immune response to vaccination with a previously unencountered HIV-1 antigen.

Authors

Suzanne L. Campion, Elena Brenna, Elaine Thomson, Will Fischer, Kristin Ladell, James E. McLaren, David A. Price, Nicole Frahm, Juliana M. McElrath, Kristen W. Cohen, Janine R. Maenza, Stephen R. Walsh, Lindsey R. Baden, Barton F. Haynes, Bette Korber, Persephone Borrow, Andrew J. McMichael

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Figure 4

Clonotype representation in the preimmunization and postvaccination repertoires of Env-reactive CD4+ T cells.

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Clonotype representation in the preimmunization and postvaccination repe...
(A) CD4+ T cell clones were derived from preimmunization repertoires (V2) of 2 volunteers, 106-009 and 106-039, who showed matching postvaccination responses to ConS peptides (V7). Expressed TRA and TRB gene rearrangements were sequenced from mRNA. (B) Protein-level expression of the corresponding TCR Vβ segments at each time point determined by flow cytometry. Plots are gated on live CD3+ cells. (C) The postvaccination TCR Vβ–defined populations shown in B were isolated by FACS to purity. Expressed TRB gene rearrangements were sequenced from mRNA. Each pie chart segment represents a distinct clonotype and the matching clonotype sequences from A.