Macaque studies of correlates of HIV protection

Mascola, John

Abstract

Current HIV vaccine candidates elicit reasonably potent cellular immune responses, but only low levels of neutralizing antibodies. Such CTL based vaccines (e.g., those based on DNA immunization) do not prevent infection, but can have a beneficial effect on disease course. In contrast, passively infused antibodies can provide complete protection, but must be administered in doses that result in serum antibody levels much higher than can be generated by current immunization strategies. We are studying the effect of passively transferred neutralizing antibodies alone, or in combination with active cellular immunity inducted by vaccination.

Funding Agency

Agency: National Institute of Health (NIH)
Institute: National Institute of Allergy and Infectious Diseases (NIAID)
Type: Intramural Research (Z01)
Project #: 1Z01AI005009-04
Application #: 7174910
Study Section: (BSL)

Project Start
Project End
Budget Start
Budget End
Support Year: 4
Fiscal Year: 2005
Total Cost
Indirect Cost

Institution

Name: Niaid Extramural Activities
Department
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DUNS #

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Country: United States
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Related projects


NIH 2008 Z01 AI	Non Human Primate Models of SIV and HIV Immune Protection Mascola, John R. / National Institute of Allergy and Infectious Diseases	$305,129
NIH 2007 Z01 AI	Non Human Primate Models of SIV and HIV Immune Protection Mascola, John R. / National Institute of Allergy and Infectious Diseases	$217,899
NIH 2006 Z01 AI	Macaque studies of correlates of HIV protection Mascola, John R. / Niaid Extramural Activities
NIH 2005 Z01 AI	Macaque studies of correlates of HIV protection Mascola, John R. / Niaid Extramural Activities
NIH 2004 Z01 AI	Macaque studies of correlates of HIV protection Mascola, John R. / Niaid Extramural Activities
NIH 2003 Z01 AI	Passive Antibody Protection In The Setting Of Active Cel Mascola, John R. / Niaid Extramural Activities
NIH 2002 Z01 AI	Passive Antibody Protection In The Setting Of Active Cel Mascola, John R. / Niaid Extramural Activities

Publications

Keele, Brandon F; Li, Hui; Learn, Gerald H et al. (2009) Low-dose rectal inoculation of rhesus macaques by SIVsmE660 or SIVmac251 recapitulates human mucosal infection by HIV-1. J Exp Med 206:1117-34

Whitney, James B; Luedemann, Corinne; Hraber, Peter et al. (2009) T-cell vaccination reduces simian immunodeficiency virus levels in semen. J Virol 83:10840-3

Letvin, Norman L; Rao, Srini S; Dang, Vi et al. (2007) No evidence for consistent virus-specific immunity in simian immunodeficiency virus-exposed, uninfected rhesus monkeys. J Virol 81:12368-74

Letvin, Norman L; Mascola, John R; Sun, Yue et al. (2006) Preserved CD4+ central memory T cells and survival in vaccinated SIV-challenged monkeys. Science 312:1530-3

Sun, Yue; Schmitz, Jorn E; Buzby, Adam P et al. (2006) Virus-specific cellular immune correlates of survival in vaccinated monkeys after simian immunodeficiency virus challenge. J Virol 80:10950-6

Acierno, Paula M; Schmitz, Jorn E; Gorgone, Darci A et al. (2006) Preservation of functional virus-specific memory CD8+ T lymphocytes in vaccinated, simian human immunodeficiency virus-infected rhesus monkeys. J Immunol 176:5338-45

Mascola, John R; Sambor, Anna; Beaudry, Kristin et al. (2005) Neutralizing antibodies elicited by immunization of monkeys with DNA plasmids and recombinant adenoviral vectors expressing human immunodeficiency virus type 1 proteins. J Virol 79:771-9

Sun, Yue; Schmitz, Jorn E; Acierno, Paula M et al. (2005) Dysfunction of simian immunodeficiency virus/simian human immunodeficiency virus-induced IL-2 expression by central memory CD4+ T lymphocytes. J Immunol 174:4753-60

Seaman, Michael S; Santra, Sampa; Newberg, Michael H et al. (2005) Vaccine-elicited memory cytotoxic T lymphocytes contribute to Mamu-A*01-associated control of simian/human immunodeficiency virus 89.6P replication in rhesus monkeys. J Virol 79:4580-8

Zhang, Lei; Ribeiro, Ruy M; Mascola, John R et al. (2004) Effects of antibody on viral kinetics in simian/human immunodeficiency virus infection: implications for vaccination. J Virol 78:5520-2

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