Abstract

application) Hepatitis C Virus (HCV) persists in more than 80% of those initially infected and over the course of decades causes chronic liver disease that can be associated to hepatocellular carcinoma, cryoglobulinemia and autoimmunity. Immune responses to HCV have been studied at the antibody, CD4, and CD8 levels in both the peripheral blood and the liver. Strong antibody responses are observed to all HCV proteins and both helper and cytotoxic T-cells have been isolated from each site of infection. Despite such evidence of immune recognition, the mechanisms by which HCV establishes and maintains infection are not well understood. Speculation that chronic HCV infection may arise from several different mechanisms is based on a number of observations that include evidence of immune deviation and generation of escape variants, neither of which is mutually exclusive. Type 2 cytokines have been observed in the serum of chronically infected patients and studies with peripheral blood T-cells have shown that HCV antigen stimulation often results in secretion of Type 2 cytokines. Paradoxically, studies in the liver suggest that local production of Th1-associated cytokines correlates with progressive hepatic damage. Because of many such similar findings in a variety of models, responses in the peripheral blood are often discounted as irrelevant to site-specific immune responses. Recognizing that HCV also infects peripheral blood mononuclear cells, however, it may be possible to reconcile such disparate results if it is postulated that the peripheral blood provides a source for constant re-infection of the liver and thus also, chronic viral persistence. Therefore, an understanding of peripheral immune responses to HCV is also critical to understanding viral immunopathogenesis. Our hypothesis is that the evasive mechanisms used by HCV arise from intrinsic hypermutability in T-cell epitopes encoded throughout the genome and that under host immune selection, there is an accumulation of HCV quasispecies expressing functionally tolerogenic epitopes conducive to viral persistence. We further postulate that in the evolutionary process by which such functionally tolerogenic epitopes are selected, helper T-cell responses shift towards a Th2 phenotype favoring chronic infection and creating a tolerogenic bias that specifically dampens effective anti-HCV responses. We believe that understanding the structural constraints upon helper T-cell interactions with functionally distinct HCV epitopes provides a powerful vantage point from which to study immune regulation in humans, our primary interest, and also leads to strategies for intervening in the infectious process.
Our aims are to examine the relationship between viral mutation and functionally distinct helper T-cell epitopes that stimulate production of different cytokines; to determine the mechanism of IL-2 suppression in response to an immunodominant epitope within the non-structural (NS) 3 protein antigen of HCV.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Scientist Development Award - Research & Training (K01)
Project #
7K01DK002970-02
Application #
6549737
Study Section
Diabetes, Endocrinology and Metabolic Diseases B Subcommittee (DDK)
Program Officer
Podskalny, Judith M,
Project Start
2001-06-01
Project End
2004-05-31
Budget Start
2001-10-01
Budget End
2002-05-31
Support Year
2
Fiscal Year
2001
Total Cost
$45,881
Indirect Cost

  Institution

Name
University of Illinois at Chicago
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
121911077
City
Chicago
State
IL
Country
United States
Zip Code
60612

  Publications

Robertson, Ruairi C; Kaliannan, Kanakaraju; Strain, Conall R et al. (2018) Maternal omega-3 fatty acids regulate offspring obesity through persistent modulation of gut microbiota. Microbiome 6:95
Oseroff, Carla; Christensen, Lars H; Westernberg, Luise et al. (2017) Immunoproteomic analysis of house dust mite antigens reveals distinct classes of dominant T cell antigens according to function and serological reactivity. Clin Exp Allergy 47:577-592
Ryan, Paul M; London, Lis E E; Bjorndahl, Trent C et al. (2017) Microbiome and metabolome modifying effects of several cardiovascular disease interventions in apo-E-/- mice. Microbiome 5:30
Oseroff, Carla; Pham, John; Frazier, April et al. (2016) Immunodominance in allergic T-cell reactivity to Japanese cedar in different geographic cohorts. Ann Allergy Asthma Immunol 117:680-689.e1
Pham, J; Oseroff, C; Hinz, D et al. (2016) Sequence conservation predicts T cell reactivity against ragweed allergens. Clin Exp Allergy 46:1194-205
Wang, Jane H; Pianko, Matthew J; Ke, Xiaogang et al. (2011) Characterization of antigenic variants of hepatitis C virus in immune evasion. Virol J 8:377
Wang, Jane H; Zheng, Xin; Ke, Xiaogang et al. (2009) Ethnic and geographical differences in HLA associations with the outcome of hepatitis C virus infection. Virol J 6:46
Wang, Jane H; Layden, Thomas J; Eckels, David D (2003) Modulation of the peripheral T-Cell response by CD4 mutants of hepatitis C virus: transition from a Th1 to a Th2 response. Hum Immunol 64:662-73
Wang, Huiru; Bian, Tonghua; Merrill, Stephen J et al. (2002) Sequence variation in the gene encoding the nonstructural 3 protein of hepatitis C virus: evidence for immune selection. J Mol Evol 54:465-73