Abstract

PROJECT 4: In nonhuman primate models of SIV infection, several studies have shown the importance of early CTL responses directed against certain epitopic regions which may lead to pressurized escape mutation, and the failure of a vaccine study due to escape mutation highlights the importance of understanding the earliest adaptive T cell pressures on virus sequence. A virus transmitted has already been passaged and shaped by the immune responses of the original host, and selection, transmission, and reversion of CTL escape mutations can occur.
In specific aim #1 we will longitudinally study, at an individual epitope-specific level, the fate of epitope-specific responses in relation to viral sequence in partner recipients also studied in Project 1. The transmitting virus and HLA type of the source party will be known, as will the HLA type of the recipient. We predict that in addition to the cost in replication capacity of a CTL escape ' mutation that will be examined in Project 1, the reversion of a CTL epitope will depend upon whether the escape mutation is recognized as a target epitope in the new host. In a detailed study of 30 HLA typed partner pairs, we will longitudinally follow recognition of HIV-gag regions rich in CTL epitopes (p17andp24) using autologous peptides. In 10 subjects we will examine responses to whole genomes. For each pair, we will (a) determine the time to escape from wild type virus for epitopes not restricted by alleles shared with the source, (b) determine the time to reversion to wild type (or not)from escape mutant transmitted virus, and (c) ascertain whether reemergence of the escape mutation occurs (""""""""re-escape""""""""). Once transmission has occurred, subjects may continue to be exposed to new viruses. Available case reports suggest that superinfection occurs primarily in recent seroconverters, and superinfection has not been observed in large cohorts of persons with established infections. Our preliminary evidence suggests that T cell responses are present to some epitopes present in both the original and superinfecting virus, while other epitopes are present only in the original virus but are altered in the superinfecting virus. The quality of the CTL response may be critical in determining whether superinfection occurs.
In specific aim #2 we will determine CTL responses to autologous epitopes in both the original and superinfecting viral variants to ascertain the characteristics of T cell responses which are effective or ineffective against the superinfecting virus. These results will be critical in advancing our ability to distinguish protective from ineffective CTL responses toHIV.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
1P01AI071713-01A1
Application #
7303509
Study Section
Special Emphasis Panel (ZAI1-ELB-A (J1))
Project Start
2007-04-01
Project End
2012-08-31
Budget Start
2007-04-01
Budget End
2008-08-31
Support Year
1
Fiscal Year
2007
Total Cost
$307,008
Indirect Cost

  Institution

Name
University of California San Francisco
Department
Type
DUNS #
094878337
City
San Francisco
State
CA
Country
United States
Zip Code
94143

  Publications

Grebe, Eduard; Welte, Alex; Hall, Jake et al. (2017) Infection Staging and Incidence Surveillance Applications of High Dynamic Range Diagnostic Immuno-Assay Platforms. J Acquir Immune Defic Syndr 76:547-555
Kassanjee, Reshma; Pilcher, Christopher D; Busch, Michael P et al. (2016) Viral load criteria and threshold optimization to improve HIV incidence assay characteristics. AIDS 30:2361-71
Keating, Sheila M; Kassanjee, Reshma; Lebedeva, Mila et al. (2016) Performance of the Bio-Rad Geenius HIV1/2 Supplemental Assay in Detecting ""Recent"" HIV Infection and Calculating Population Incidence. J Acquir Immune Defic Syndr 73:581-588
Wright, Patrick W; Pyakurel, Ashmit; Vaida, Florin F et al. (2016) Putamen volume and its clinical and neurological correlates in primary HIV infection. AIDS 30:1789-94
Pinzone, Marilia Rita; Graf, Erin; Lynch, Lindsay et al. (2016) Monitoring Integration over Time Supports a Role for Cytotoxic T Lymphocytes and Ongoing Replication as Determinants of Reservoir Size. J Virol 90:10436-10445
Pilcher, Christopher D; Bisol, Claudia Alquati; Paganella, Machline Paim et al. (2015) Efficient Identification of HIV Serodiscordant Couples by Existing HIV Testing Programs in South Brazil. PLoS One 10:e0142638
Vujkovic-Cvijin, Ivan; Swainson, Louise A; Chu, Simon N et al. (2015) Gut-Resident Lactobacillus Abundance Associates with IDO1 Inhibition and Th17 Dynamics in SIV-Infected Macaques. Cell Rep 13:1589-97
Hollingsworth, T Déirdre; Pilcher, Christopher D; Hecht, Frederick M et al. (2015) High Transmissibility During Early HIV Infection Among Men Who Have Sex With Men-San Francisco, California. J Infect Dis 211:1757-60
Kassanjee, Reshma; Pilcher, Christopher D; Keating, Sheila M et al. (2014) Independent assessment of candidate HIV incidence assays on specimens in the CEPHIA repository. AIDS 28:2439-49
Michaud, Henri-Alexandre; SenGupta, Devi; de Mulder, Miguel et al. (2014) Cutting edge: An antibody recognizing ancestral endogenous virus glycoproteins mediates antibody-dependent cellular cytotoxicity on HIV-1-infected cells. J Immunol 193:1544-8

Showing the most recent 10 out of 46 publications