Safety and immunogenicity of an HIV adenoviral vector boost after DNA plasmid vaccine prime by route of administration: a randomized clinical trial

Beryl A Koblin; Martin Casapia; Cecilia Morgan; Li Qin; Zhixue Maggie Wang; Olivier D Defawe; Lindsey Baden; Paul Goepfert; Georgia D Tomaras; David C Montefiori; M Juliana McElrath; Lilian Saavedra; Chuen-Yen Lau; Barney S Graham; NIAID HIV Vaccine Trials Network

doi:10.1371/journal.pone.0024517

Safety and immunogenicity of an HIV adenoviral vector boost after DNA plasmid vaccine prime by route of administration: a randomized clinical trial

PLoS One. 2011;6(9):e24517. doi: 10.1371/journal.pone.0024517. Epub 2011 Sep 12.

Authors

Beryl A Koblin¹, Martin Casapia, Cecilia Morgan, Li Qin, Zhixue Maggie Wang, Olivier D Defawe, Lindsey Baden, Paul Goepfert, Georgia D Tomaras, David C Montefiori, M Juliana McElrath, Lilian Saavedra, Chuen-Yen Lau, Barney S Graham; NIAID HIV Vaccine Trials Network

Affiliation

¹ Laboratory of Infectious Disease Prevention, New York Blood Center, New York, New York, United States of America. bkoblin@nybloodcenter.org

Abstract

Background: In the development of HIV vaccines, improving immunogenicity while maintaining safety is critical. Route of administration can be an important factor.

Methodology/principal findings: This multicenter, open-label, randomized trial, HVTN 069, compared routes of administration on safety and immunogenicity of a DNA vaccine prime given intramuscularly at 0, 1 and 2 months and a recombinant replication-defective adenovirus type 5 (rAd5) vaccine boost given at 6 months by intramuscular (IM), intradermal (ID), or subcutaneous (SC) route. Randomization was computer-generated by a central data management center; participants and staff were not blinded to group assignment. The outcomes were vaccine reactogenicity and humoral and cellular immunogenicity. Ninety healthy, HIV-1 uninfected adults in the US and Peru, aged 18-50 were enrolled and randomized. Due to the results of the Step Study, injections with rAd5 vaccine were halted; thus 61 received the booster dose of rAd5 vaccine (IM: 20; ID:21; SC:20). After the rAd5 boost, significant differences by study arm were found in severity of headache, pain and erythema/induration. Immune responses (binding and neutralizing antibodies, IFN-γ ELISpot HIV-specific responses and CD4+ and CD8+ T-cell responses by ICS) at four weeks after the rAd5 booster were not significantly different by administration route of the rAd5 vaccine boost (Binding antibody responses: IM: 66.7%; ID: 70.0%; SC: 77.8%; neutralizing antibody responses: IM: 11.1%; ID: 0.0%; SC 16.7%; ELISpot responses: IM: 46.7%; ID: 35.3%; SC: 44.4%; CD4+ T-cell responses: IM: 29.4%; ID: 20.0%; SC: 35.3%; CD8+ T-cell responses: IM: 29.4%; ID: 16.7%; SC: 50.0%.)

Conclusions/significance: This study was limited by the reduced sample size. The higher frequency of local reactions after ID and SC administration and the lack of sufficient evidence to show that there were any differences in immunogenicity by route of administration do not support changing route of administration for the rAd5 boost.

Trial registration: ClinicalTrials.gov NCT00384787.

Publication types

Multicenter Study
Randomized Controlled Trial
Research Support, N.I.H., Extramural

MeSH terms

AIDS Vaccines / therapeutic use*
Adenoviridae / genetics*
Adolescent
Adult
Cytokines / metabolism
DNA / genetics*
Female
Genetic Vectors
HIV / genetics*
HIV Infections / prevention & control*
Humans
Immunoenzyme Techniques / methods
Male
Middle Aged
Neutralization Tests
Plasmids / metabolism
Time Factors
Vaccines, DNA / therapeutic use*

Substances

AIDS Vaccines
Cytokines
Vaccines, DNA
DNA

Associated data

ClinicalTrials.gov/NCT00384787

Grants and funding

U01 AI068618/AI/NIAID NIH HHS/United States