Comparative Seroprevalence and Immunogenicity of Six Rare Serotype Recombinant Adenovirus Vaccine Vectors from Subgroups B and D

doi:10.1128/JVI.02696-06

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Journal of Virology, May 2007, p. 4654-4663, Vol. 81, No. 9
0022-538X/07/$08.00+0 doi:10.1128/JVI.02696-06
Copyright © 2007, American Society for Microbiology. All Rights Reserved.

Comparative Seroprevalence and Immunogenicity of Six Rare Serotype Recombinant Adenovirus Vaccine Vectors from Subgroups B and D

Peter Abbink,¹ Angelique A. C. Lemckert,² Bonnie A. Ewald,¹ Diana M. Lynch,¹ Matthew Denholtz,¹ Shirley Smits,² Lennart Holterman,² Irma Damen,² Ronald Vogels,² Anna R. Thorner,¹ Kara L. O'Brien,¹ Angela Carville,³ Keith G. Mansfield,³ Jaap Goudsmit,² Menzo J. E. Havenga,² and Dan H. Barouch¹^*

Division of Viral Pathogenesis, Beth Israel Deaconess Medical Center, Harvard Medical School, Boston, Massachusetts 02215,¹ Crucell Holland BV, 2301 CA, Leiden, The Netherlands,² New England Primate Research Center, Southborough, Massachusetts 01772³

Received 6 December 2006/ Accepted 17 February 2007

Recombinant adenovirus serotype 5 (rAd5) vector-based vaccinesare currently being developed for both human immunodeficiencyvirus type 1 and other pathogens. The potential limitationsassociated with rAd5 vectors, however, have led to the constructionof novel rAd vectors derived from rare Ad serotypes. Severalrare serotype rAd vectors have already been described, but adetailed comparison of multiple rAd vectors from subgroups Band D has not previously been reported. Such a comparison iscritical for selecting optimal rAd vectors for advancement intoclinical trials. Here we describe the construction of threenovel rAd vector systems from Ad26, Ad48, and Ad50. We reportcomparative seroprevalence and immunogenicity studies involvingrAd11, rAd35, and rAd50 vectors from subgroup B; rAd26, rAd48,and rAd49 vectors from subgroup D; and rAd5 vectors from subgroupC. All six rAd vectors from subgroups B and D exhibited lowseroprevalence in a cohort of 200 individuals from sub-SaharanAfrica, and they elicited Gag-specific cellular immune responsesin mice both with and without preexisting anti-Ad5 immunity.The rAd vectors from subgroup D were also evaluated using rhesusmonkeys and were shown to be immunogenic after a single injection.The rAd26 vectors proved the most immunogenic among the rareserotype rAd vectors studied, although all rare serotype rAdvectors were still less potent than rAd5 vectors in the absenceof anti-Ad5 immunity. These studies substantially expand theportfolio of rare serotype rAd vectors that may prove usefulas vaccine vectors for the developing world.

* Corresponding author. Mailing address: Research East Room 213, Division of Viral Pathogenesis, Beth Israel Deaconess Medical Center, 330 Brookline Avenue, Boston, MA 02215. Phone: (617) 667-4434. Fax: (617) 667-8210. E-mail: dbarouch{at}bidmc.harvard.edu

Published ahead of print on 28 February 2007.

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