Immunogenicity of Recombinant Adenovirus Serotype 35 Vaccine in the Presence of Pre-existing Anti-Ad5 Immunity

Overview

Journal J Immunol

Specialty Allergy & Immunology

Date 2004 May 7

PMID 15128818

Citations 201

Authors

Dan H Barouch

Maria G Pau

Jerome H H V Custers

Wouter Koudstaal

Stefan Kostense

Menzo J E Havenga

Diana M Truitt

Shawn M Sumida

Michael G Kishko

Janelle C Arthur

Birgit Korioth-Schmitz

Michael H Newberg

Darci A Gorgone

Michelle A Lifton

Dennis L Panicali

Gary J Nabel

Norman L Letvin

Jaap Goudsmit

Affiliations

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Abstract

The high prevalence of pre-existing immunity to adenovirus serotype 5 (Ad5) in human populations may substantially limit the immunogenicity and clinical utility of recombinant Ad5 vector-based vaccines for HIV-1 and other pathogens. A potential solution to this problem is to use vaccine vectors derived from adenovirus (Ad) serotypes that are rare in humans, such as Ad35. However, cross-reactive immune responses between heterologous Ad serotypes have been described and could prove a major limitation of this strategy. In particular, the extent of immunologic cross-reactivity between Ad5 and Ad35 has not previously been determined. In this study we investigate the impact of pre-existing anti-Ad5 immunity on the immunogenicity of candidate rAd5 and rAd35 vaccines expressing SIV Gag in mice. Anti-Ad5 immunity at levels typically found in humans dramatically blunted the immunogenicity of rAd5-Gag. In contrast, even high levels of anti-Ad5 immunity did not substantially suppress Gag-specific cellular immune responses elicited by rAd35-Gag. Low levels of cross-reactive Ad5/Ad35-specific CD4(+) T lymphocyte responses were observed, but were insufficient to suppress vaccine immunogenicity. These data demonstrate the potential utility of Ad35 as a candidate vaccine vector that is minimally suppressed by anti-Ad5 immunity. Moreover, these studies suggest that using Ad vectors derived from immunologically distinct serotypes may be an effective and general strategy to overcome the suppressive effects of pre-existing anti-Ad immunity.

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