Abstract

The goal of Research Project III (Evaluation of AFE inhibitors for protection from SHIV vaginal challenge in macaques) is to evaluate the safety and potency of suitably formulated combinations of AFE inhibitors in the rhesus macaque vaginal challenge model. The Leader will be Ronald Veazey, DVM, PhD, at the Tulane National Primate Research Center, Tulane, LA. We will receive inhibitors and formulations from Core A after confirmation of their potency and non-toxicity in the in vitro models (Research Projects I and II, and Core A). We will examine the safety of the inhibitors and formulations after topical application to the macaque vagina, by performing colposcopy and vaginal biopsy after repeated vaginal administrations of the drugs, to ensure they do not cause local inflammatory responses. Inhibitors with suitable safety profiles will be assessed, alone and in combination, for their ability to prevent the vaginal transmission of the R5 SHIV-162P3 challenge virus, and/or the X4 virus SHIV-89.6P. The outcome of infection will be determined by measuring plasma viremia and confirmed by Western blots for anti-viral antibodies. We may also explore the ability of selected inhibitors to prevent vaginal transmission, or to counter established infection, after systemic or oral administration, if we judge it likely that this information will assist us in evaluating safety and toxicity profiles. For efficacy studies, we will primarily use progesterone-treated macaques, in which the vaginal epithelium is thinned prior to vaginal challenge. This enables us to infect >90% of control animals with a relatively low challenge dose (300 TCID50). This model will also be used for evaluating compound safety as the thin vaginal epithelium allows much more sensitive detection of vaginal inflammation. However, we will also explore the potential of the multiple, low dose vaginal challenge model, administering a much lower dose (10 TCID50) of virus weekly to macaques without prior progesterone treatment. These studies will help identify the most suitable AFE inhibitors for advancement into human safety trials in Research Project IV.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program--Cooperative Agreements (U19)
Project #
5U19AI065413-02
Application #
7310317
Study Section
Special Emphasis Panel (ZRG1)
Project Start
Project End
Budget Start
2006-08-01
Budget End
2007-07-31
Support Year
2
Fiscal Year
2006
Total Cost
$612,233
Indirect Cost

  Institution

Name
Weill Medical College of Cornell University
Department
Type
DUNS #
060217502
City
New York
State
NY
Country
United States
Zip Code
10065

  Publications

Ingallinella, Paolo; Bianchi, Elisabetta; Ladwa, Neal A et al. (2009) Addition of a cholesterol group to an HIV-1 peptide fusion inhibitor dramatically increases its antiviral potency. Proc Natl Acad Sci U S A 106:5801-6
Pahar, Bapi; Lackner, Andrew A; Piatak Jr, Michael et al. (2009) Control of viremia and maintenance of intestinal CD4(+) memory T cells in SHIV(162P3) infected macaques after pathogenic SIV(MAC251) challenge. Virology 387:273-84
Vachot, Laurence; Williams, Vennansha G; Bess Jr, Julian W et al. (2008) Candida albicans-induced DC activation partially restricts HIV amplification in DCs and increases DC to T-cell spread of HIV. J Acquir Immune Defic Syndr 48:398-407
Frank, I; Stossel, H; Gettie, A et al. (2008) A fusion inhibitor prevents spread of immunodeficiency viruses, but not activation of virus-specific T cells, by dendritic cells. J Virol 82:5329-39
Veazey, Ronald S; Ketas, Thomas A; Klasse, Per Johan et al. (2008) Tropism-independent protection of macaques against vaginal transmission of three SHIVs by the HIV-1 fusion inhibitor T-1249. Proc Natl Acad Sci U S A 105:10531-6
Veazey, Ronald S (2008) Microbicide safety/efficacy studies in animals: macaques and small animal models. Curr Opin HIV AIDS 3:567-73
Turville, Stuart G; Aravantinou, Meropi; Stossel, Hella et al. (2008) Resolution of de novo HIV production and trafficking in immature dendritic cells. Nat Methods 5:75-85
Klasse, Per Johan; Shattock, Robin; Moore, John P (2008) Antiretroviral drug-based microbicides to prevent HIV-1 sexual transmission. Annu Rev Med 59:455-71
Hu, Qinxue; Mahmood, Naheed; Shattock, Robin J (2007) High-mannose-specific deglycosylation of HIV-1 gp120 induced by resistance to cyanovirin-N and the impact on antibody neutralization. Virology 368:145-54
Ketas, Thomas J; Kuhmann, Shawn E; Palmer, Ashley et al. (2007) Cell surface expression of CCR5 and other host factors influence the inhibition of HIV-1 infection of human lymphocytes by CCR5 ligands. Virology 364:281-90

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