Abstract

The long-range goal of this HIVRAD Program Project is to develop vaccine strategies against mucosalHIV clade C transmission, with a special focus on identifying conserved regions on HIV clade C envelopeglycoproteins that are targets for neutralizing antibodies (nAbs). The overall objectives for Core C (Primate Studies) are to provide the experimental animals and supportservices needed to facilitate the efficient completion of the aims outlined in Project 1 and Core A (molecularevolution of HIV clade C envelope genes in humans and primates), Project 2 (isolating neutralizingmonoclonal antibodies and mimotopes), and Project 3 (recombinant replication-competent adenovirusprime/protein boost vaccination). This will include the provision of retrovirus-free juvenile and infant rhesusmacaques from the Yerkes rhesus macaque breeding colonies; adaptation of novel chimeric simian-humanimmunodeficiency virus (SHIV) constructs that encode various HIV clade C env genes (SHIVenvC strains) torhesus macaques (Core A); titration of SHIVenvC strains by the intrarectal and oral routes to provide vaccinechallenge stocks (Project 3) and assessment of viral pathogenicity in infant and juvenile animals; collectionof blood and bone marrow samples from monkeys with broadly reactive nAb responses (Project 2); andimmunization and mucosal challenges of rhesus monkeys (Project 3). Core C tasks also include dailymonitoring of the experimental animals; periodic physical examinations with blood collections forimmunologic and virologic evaluations and shipment of samples to the Program Project investigators; theperformance of CBCs and flow cytometry evaluation to determine lymphocyte subsets; and the performanceof a basic gross and histologic necropsy evaluations of all experimental animals that die or are sacrificedduring the course of this study. Provision of these resources and support services will facilitate the development and testing of the novelAIDS vaccine concepts proposed in this Program Project. Core C studies will play a key role in theestablishment of a biologically relevant R5 SHIVenvC model of mucosal transmission and pathogenicity, andwill allow evaluation of vaccine efficacy with either prevention of infection (sterilizing immunity) or significantmodulation of post-challenge viral loads and immunological parameters as criteria of vaccine efficacy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
5P01AI048240-07
Application #
7676658
Study Section
Special Emphasis Panel (ZAI1)
Project Start
2008-08-01
Project End
2012-07-31
Budget Start
2008-08-01
Budget End
2009-07-31
Support Year
7
Fiscal Year
2008
Total Cost
$719,755
Indirect Cost

  Institution

Name
Dana-Farber Cancer Institute
Department
Type
DUNS #
076580745
City
Boston
State
MA
Country
United States
Zip Code
02215

  Publications

Tokatlian, Talar; Kulp, Daniel W; Mutafyan, Andrew A et al. (2018) Enhancing Humoral Responses Against HIV Envelope Trimers via Nanoparticle Delivery with Stabilized Synthetic Liposomes. Sci Rep 8:16527
Ruprecht, Ruth M; Lakhashe, Samir K (2017) Antibody-mediated immune exclusion of HIV. Curr Opin HIV AIDS 12:222-228
Ruprecht, Ruth M (2017) Anti-HIV Passive Immunization: New Weapons in the Arsenal. Trends Microbiol 25:954-956
Schneider, Jeffrey R; Carias, Ann M; Bastian, Arangaserry R et al. (2017) Long-term direct visualization of passively transferred fluorophore-conjugated antibodies. J Immunol Methods 450:66-72
Kulkarni, Viraj; Ruprecht, Ruth M (2017) Mucosal IgA Responses: Damaged in Established HIV Infection-Yet, Effective Weapon against HIV Transmission. Front Immunol 8:1581
Sholukh, Anton M; Watkins, Jennifer D; Vyas, Hemant K et al. (2015) Defense-in-depth by mucosally administered anti-HIV dimeric IgA2 and systemic IgG1 mAbs: complete protection of rhesus monkeys from mucosal SHIV challenge. Vaccine 33:2086-95
Lakhashe, Samir K; Byrareddy, Siddappa N; Zhou, Mingkui et al. (2014) Multimodality vaccination against clade C SHIV: partial protection against mucosal challenges with a heterologous tier 2 virus. Vaccine 32:6527-36
Zhou, Mingkui; Ruprecht, Ruth M (2014) Are anti-HIV IgAs good guys or bad guys? Retrovirology 11:109
Sholukh, Anton M; Byrareddy, Siddappa N; Shanmuganathan, Vivekanandan et al. (2014) Passive immunization of macaques with polyclonal anti-SHIV IgG against a heterologous tier 2 SHIV: outcome depends on IgG dose. Retrovirology 11:8
Bachler, Barbara C; Humbert, Michael; Lakhashe, Samir K et al. (2013) Live-virus exposure of vaccine-protected macaques alters the anti-HIV-1 antibody repertoire in the absence of viremia. Retrovirology 10:63

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