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    Date Issued2008 (3)AuthorGreen, Sharone (3)Kennedy, Jeffrey S. (3)Lu, Shan (3)
    Markham, Phillip (3)
    Pal, Ranajit (3)View MoreUMass Chan AffiliationCenter for Infectious Disease and Vaccine Research (2)Department of Medicine, Division of Infectious Diseases and Immunology (2)Laboratory of Nucleic Acid Vaccines (2)Department of Anesthesiology (1)Document TypeJournal Article (3)KeywordAdult (2)AIDS Vaccines (2)Human Experimentation (2)Humans (2)Life Sciences (2)View MoreJournalVaccine (3)

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    Cross-subtype antibody and cellular immune responses induced by a polyvalent DNA prime-protein boost HIV-1 vaccine in healthy human volunteers

    Wang, Shixia; Kennedy, Jeffrey S.; West, Kim; Montefiori, David C.; Coley, Scott; Lawrence, John; Shen, Siyuan; Green, Sharone; Rothman, Alan L.; Ennis, Francis A.; et al. (2008-07-23)
    An optimally effective AIDS vaccine would likely require the induction of both neutralizing antibody and cell-mediated immune responses, which has proven difficult to obtain in previous clinical trials. Here we report on the induction of human immunodeficiency virus type-1 (HIV-1)-specific immune responses in healthy adult volunteers that received the multi-gene, polyvalent, DNA prime-protein boost HIV-1 vaccine formulation, DP6-001, in a Phase I clinical trial. Robust cross-subtype HIV-1 specific T cell responses were detected in IFN-gamma ELISPOT assays. Furthermore, we detected high titer serum antibody responses that recognized a wide range of primary HIV-1 Env antigens and also neutralized pseudotyped viruses that express the primary Env antigens from multiple HIV-1 subtypes. These findings demonstrate that the DNA prime-protein boost approach is an effective immunization method to elicit both humoral and cell-mediated immune responses in humans, and that a polyvalent Env formulation could generate broad immune responses against HIV-1 viruses with diverse genetic backgrounds.
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    The safety and tolerability of an HIV-1 DNA prime-protein boost vaccine (DP6-001) in healthy adult volunteers

    Kennedy, Jeffrey S.; Co, Mary Dawn T.; Green, Sharone; Longtine, Karen J.; Longtine, Jaclyn K.; O'Neill, Melissa A.; Adams, Janice P.; Rothman, Alan L.; Yu, Qiao; Johnson-Leva, Renita; et al. (2008-07-01)
    This report describes the safety observations following administration of a polyvalent DNA prime-protein boost HIV-1 vaccine formulated with adjuvant QS21. Local injection site reactions were the most common (65% of subjects), and included type IV delayed-type hypersensitivity (DTH) reactions at prior DNA inoculation sites in 12 of 28 (43%) subjects following protein vaccination. Systemic reactions revealed two cases of vasculitis temporally related to inoculation with recombinant Env protein+QS21 adjuvant. Questions remain regarding the cause of the vasculitis, but the unique DTH observation may have contributed to the high level of immune responses previously reported for this vaccine.
    Thumbnail

    Cross-subtype antibody and cellular immune responses induced by a polyvalent DNA prime-protein boost HIV-1 vaccine in healthy human volunteers

    Wang, Shixia; Kennedy, Jeffrey S.; West, Kim; Montefiori, David C.; Coley, Scott E.; Lawrence, John M.; Shen, Siyuan; Green, Sharone; Rothman, Alan L.; Ennis, Francis A.; et al. (2008-02-05)
    An optimally effective AIDS vaccine would likely require the induction of both neutralizing antibody and cell-mediated immune responses, which has proven difficult to obtain in previous clinical trials. Here we report on the induction of Human Immunodeficiency Virus Type-1 (HIV-1)-specific immune responses in healthy adult volunteers that received the multi-gene, polyvalent, DNA prime-protein boost HIV-1 vaccine formulation, DP6-001, in a Phase I clinical trial conducted in healthy adult volunteers of both genders. Robust cross-subtype HIV-1-specific T cell responses were detected in IFNgamma ELISPOT assays. Furthermore, we detected high titer serum antibody responses that recognized a wide range of primary HIV-1 Env antigens and also neutralized pseudotyped viruses that express the primary Env antigens from multiple HIV-1 subtypes. These findings demonstrate that the DNA prime-protein boost approach is an effective immunization method to elicit both humoral and cell-mediated immune responses in humans, and that a polyvalent Env formulation could generate broad immune responses against HIV-1 viruses with diverse genetic backgrounds.
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