Abstract
The mechanisms whereby different vaccines may expand distinct Ag-specific T cell clonotypes or induce disparate degrees of protection are incompletely understood. We found that several delivery modes of a model retroviral Ag, including natural infection, preferentially expanded initially rare high-avidity CD4(+) T cell clonotypes, known to mediate protection. In contrast, the same Ag vectored by human adenovirus serotype 5 induced clonotypic expansion irrespective of avidity, eliciting a predominantly low-avidity response. Nonselective clonotypic expansion was caused by relatively weak adenovirus serotype 5-vectored Ag presentation and was reproduced by replication-attenuated retroviral vaccines. Mechanistically, the potency of Ag presentation determined the speed and, consequently, completion of the CD4(+) T cell response. Whereas faster completion retained the initial advantage of high-avidity clonotypes, slower completion permitted uninhibited accumulation of low-avidity clonotypes. These results highlighted the importance of Ag presentation patterns in determining the clonotypic composition of vaccine-induced T cell responses and ultimately the efficacy of vaccination.
Highlights
Clonotypic Composition of the CD4+ T Cell Response to a Vectored Retroviral Antigen Is Determined by Its Speed
The response to Friend virus (FV) infection was dominated (.70%) by high-avidity Va2 CD4+ T cells [23], and this was reproduced with several different immunization methods (Fig. 1A), including Friend murine leukemia virus (F-murine leukemia virus (MLV))-B, env124–138 peptide in Sigma Adjuvant System, and FV-induced FBL-3 tumor cells expressing F-MLV env
A replication-defective recombinant adenovirus serotype 5 (Ad5)–based vaccine encoding F-MLV env (Ad5.pIX-gp70) induced predominantly non–Va2 CD4+ T cells (Fig. 1A–C). Both B-tropic F-MLV (F-MLV-B) and Ad5.pIX-gp70 elicited an env-specific CD4+ T cell response of comparable magnitude (Fig. 1A, 1B), the proportion of high-avidity Va2 CD4+ T cells within this response was significantly lower for Ad5.pIX-gp70 than for F-MLV-B (Fig. 1B, 1C)
Summary
Clonotypic Composition of the CD4+ T Cell Response to a Vectored Retroviral Antigen Is Determined by Its Speed. The response to FV infection was dominated (.70%) by high-avidity Va2 CD4+ T cells [23], and this was reproduced with several different immunization methods (Fig. 1A), including F-MLV-B, env124–138 peptide in Sigma Adjuvant System, and FV-induced FBL-3 tumor cells expressing F-MLV env.
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