Abstract

The extent of CNS dysfunction observed during HIV-l infection is likely due to both host and viral factors that include but are not limited to differences in receptor and coreceptor expression, physiology of target cell populations, cytokine and chemokine expression, neurotoxicity of viral proteins such as gpl2O Tat, and Nef, functional properties of the long terminal repeat (LTR), and functional properties of the viral trans-activator proteins, Tat and Vpr. The studies proposed in this competitive renewal application will continue to examine the structural evolution of the HIV-1 LTR and its interaction with several families of cellular transcription factors and viral trans-activators (Tat and Vpr) within cells of the monocyte/macrophage lineage. Of particular importance will be studies focused on examining the relationships of these biomolecular interactions with progressive HIV-1-associated neurologic dysfunction. The GENERAL HYPOTHESIS to be tested is that the C/EBP transcription factor family, in concert with other cellular factors and the HIV-1 protein Vpr, interact with specific configurations of C/EBP sites I and II to activate viral gene expression in cells of the monocyte/macrophage lineage. Based on clinical observations, in vivo animal model studies, and in vitro tissue culture investigations performed by a number of Investigators, increased genomic expression can potentially lead to an increased CNS viral load and/or an enhanced production of viral neurotoxic proteins gp120, Tat, and/or Nef, leading to glial and/or neuronal dysfunction and CNS disease progression. We propose that evolution of the HIV-1 LTR as well as the Vpr and Tat genes within cells of the monocyte/macrophage lineage prior to or after entry into the CNS plays a critical role in the overall outcome of this process. renewal application are to examine the: (1) physical and functional interaction of the C/EBP transcription factor family with the HIV-1 LTR and other cellular factors critical to viral genome activation; (2) interaction of C/EBP factors and HIV-l Vpr with C/EBP binding sites I and II within the HIV-l LTR and the impact of sequence variation and other cellular transcription factors on these interactions; (3) interaction of HIV-1 Vpr with the viral LTR within the context of HIV-1 infectious molecular clones and primary cell populations derived from peripheral blood and CNS; (4) functional correlations between high affinity interactions of HIV-1 Vpr with specific configurations of C/EBP binding site I and HIVD; and (5) structural co-evolution of the HIV-1 LTR and Vpr gene during HIV-l CNS infection, in o propagation in cells of the monocyte/macrophage lineage, and functional correlations between LTR/Vpr co-evolution and HIVD. These studies may provide insight relevant to the development of new molecular diagnostic reagents and therapeutic strategies to monitor and control HIV-1-associated neurologic disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS032092-13
Application #
6539767
Study Section
AIDS and Related Research 8 (AARR)
Program Officer
Nunn, Michael
Project Start
1993-01-01
Project End
2003-06-30
Budget Start
2002-07-01
Budget End
2003-06-30
Support Year
13
Fiscal Year
2002
Total Cost
$342,072
Indirect Cost

  Institution

Name
Pennsylvania State University
Department
Microbiology/Immun/Virology
Type
Schools of Medicine
DUNS #
129348186
City
Hershey
State
PA
Country
United States
Zip Code
17033

  Publications

Dampier, Will; Antell, Gregory C; Aiamkitsumrit, Benjamas et al. (2017) Specific amino acids in HIV-1 Vpr are significantly associated with differences in patient neurocognitive status. J Neurovirol 23:113-124
Banerjee, Anupam; Li, Luna; Pirrone, Vanessa et al. (2017) cAMP Signaling Enhances HIV-1 Long Terminal Repeat (LTR)-directed Transcription and Viral Replication in Bone Marrow Progenitor Cells. Clin Med Insights Pathol 10:1179555717694535
Antell, Gregory C; Dampier, Will; Aiamkitsumrit, Benjamas et al. (2017) Evidence of Divergent Amino Acid Usage in Comparative Analyses of R5- and X4-Associated HIV-1 Vpr Sequences. Int J Genomics 2017:4081585
Datta, Prasun K; Kaminski, Rafal; Hu, Wenhui et al. (2016) HIV-1 Latency and Eradication: Past, Present and Future. Curr HIV Res 14:431-441
Antell, Gregory C; Dampier, Will; Aiamkitsumrit, Benjamas et al. (2016) Utilization of HIV-1 envelope V3 to identify X4- and R5-specific Tat and LTR sequence signatures. Retrovirology 13:32
Strazza, Marianne; Maubert, Monique E; Pirrone, Vanessa et al. (2016) Co-culture model consisting of human brain microvascular endothelial and peripheral blood mononuclear cells. J Neurosci Methods 269:39-45
Strazza, Marianne; Pirrone, Vanessa; Wigdahl, Brian et al. (2016) Prolonged Morphine Exposure Induces Increased Firm Adhesion in an in Vitro Model of the Blood-Brain Barrier. Int J Mol Sci 17:
Nonnemacher, Michael R; Pirrone, Vanessa; Feng, Rui et al. (2016) HIV-1 Promoter Single Nucleotide Polymorphisms Are Associated with Clinical Disease Severity. PLoS One 11:e0150835
James, Tony; Nonnemacher, Michael R; Wigdahl, Brian et al. (2016) Defining the roles for Vpr in HIV-1-associated neuropathogenesis. J Neurovirol 22:403-15
Kollias, Christina M; Huneke, Richard B; Wigdahl, Brian et al. (2015) Animal models of herpes simplex virus immunity and pathogenesis. J Neurovirol 21:8-23

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