Abstract

The purpose of this project has been to develop and characterize an in vivo transgenic mouse model for examining mechanisms of microbial induced immune activation of HIV-1 as well as for testing of candidate treatments that might block this process. Progress was achieved this year in the following areas. Continued studies on the cellular source of HIV-1 expression in spleen indicated that in addition to macrophages and dendritic cells (DC), B lymphocytes can also serve as a source of virus following microbial stimulation. A project was initiated to characterize the receptors and signalling pathways responsible for HIV induction in these splenic APC populations. This work identified TLR 2 and 4 binding microbial ligands, IL-1, IL-18, GM-CSF, CD40L and CpG oligonucleotides as agonists of HIV-expression and IL-4 and IFN alpha/beta as antagonists. CD40L stimulation was studied in detail and was shown to be largely responsible for the induction of virus from DC by polyclonally activated or Ag stimulated T lymphocytes through its interaction with CD40. Indeed, this T cell-APC interaction was shown to be a major pathway involved in the stimulation of HIV expression during experimental malaria infection. Thus, CD4 depletion or administration of a CD40L antagonist both dramatically inhibited virus production in acutely infected mice. In related work, prednisolone or an Env binding CD4-toxin conjugate, two agents previously shown by us to reduce HIV-1 expression in vitro both markedly inhibited in vivo virus production stimulated by M. avium. infection. The above observations formally establish the utility of the transgenic mouse model as a system for testing interventions that inhibit microbial induced immune activation of HIV-1 in vivo. In separate studies, it was shown that bone marrow derived DC from transgenic mice induce substantial levels of both HIV specific Ab as well as CTL activity against transfected targets when used to immunize either control FVB/N or transgenic mice. The latter observations establish a model system for developing DC based vaccination schemes against HIV.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Intramural Research (Z01)
Project #
1Z01AI000875-01
Application #
6414640
Study Section
(LPD)
Project Start
Project End
Budget Start
Budget End
Support Year
1
Fiscal Year
2000
Total Cost
Indirect Cost

  Institution

Name
Niaid Extramural Activities
Department
Type
DUNS #
City
State
Country
United States
Zip Code

  Publications

Bafica, Andre; Scanga, Charles A; Schito, Marco et al. (2004) Influence of coinfecting pathogens on HIV expression: evidence for a role of Toll-like receptors. J Immunol 172:7229-34
Bafica, Andre; Scanga, Charles A; Equils, Ozlem et al. (2004) The induction of Toll-like receptor tolerance enhances rather than suppresses HIV-1 gene expression in transgenic mice. J Leukoc Biol 75:460-6
Equils, Ozlem; Schito, Marco L; Karahashi, Hiase et al. (2003) Toll-like receptor 2 (TLR2) and TLR9 signaling results in HIV-long terminal repeat trans-activation and HIV replication in HIV-1 transgenic mouse spleen cells: implications of simultaneous activation of TLRs on HIV replication. J Immunol 170:5159-64
Schito, Marco L; Goel, Atul; Song, Yongsheng et al. (2003) In vivo antiviral activity of novel human immunodeficiency virus type 1 nucleocapsid p7 zinc finger inhibitors in a transgenic murine model. AIDS Res Hum Retroviruses 19:91-101
Bafica, Andre; Scanga, Charles A; Schito, Marco L et al. (2003) Cutting edge: in vivo induction of integrated HIV-1 expression by mycobacteria is critically dependent on Toll-like receptor 2. J Immunol 171:1123-7
Freitag, C; Chougnet, C; Schito, M et al. (2001) Malaria infection induces virus expression in human immunodeficiency virus transgenic mice by CD4 T cell-dependent immune activation. J Infect Dis 183:1260-8
Chougnet, C; Freitag, C; Schito, M et al. (2001) In vivo CD40-CD154 (CD40 ligand) interaction induces integrated HIV expression by APC in an HIV-1-transgenic mouse model. J Immunol 166:3210-7
Schito, M L; Kennedy, P E; Kowal, R P et al. (2001) A human immunodeficiency virus-transgenic mouse model for assessing interventions that block microbial-induced proviral expression. J Infect Dis 183:1592-600