Abstract

There are few animal models available for the study of hepatitis C (HCV) infection so that further understanding of the pathogenesis of liver disease associated with this infection must rely in part on studies in humans. We have the unique opportunity to examine the influence of immune response on the natural history and pathogenesis of this disease by studying three patient populations with HCV infection; liver transplant patients who have impaired T cell function, patients with common variable immunodeficiency who have impaired humoral immunity and patient with intact immune responses. Our hypotheses is that the natural history of disease differs in these three groups, and that progressive liver disease occurs more frequently in immunocompromised than in immunocompetent patients. Moreover, we propose that the effect of immune deficiency is independent of other factors which may influence disease progression, such as viral genotype and level of viral replication. Our secondary hypothesis is that viral diversity is central to the mechanism by which immune response influences disease progression. Using our three patient groups. we will examine the relationship between immune response and viral diversity, which will be measured indirectly by single stranded conformational polymorphism and directly by analysis of the sequence variation in the envelope region of HCV over time. The immune response could influence viral divergence either by selecting for or by inhibiting viral diversity. Support for the former hypothesis would be provided by finding that the rate of viral mutation is higher in immunocompetent than in immunocompromised patients. Support for the latter hypothesis would be provided by finding that the rate of viral mutation is lower in immunocompetent that in immunocompromised patients. In order to examine further the mechanism by which humoral immunity is associated with viral diversity, we will determine the time course of emergence of viral species and the production of antibodies specific for these viral isolates. Since viral diversity could influence disease progression independent of host immunity, we will examine directly the relationship between diversity and disease progression. Elucidation of the mechanisms by which HCV causes progressive disease is essential for improved understanding of the pathogenesis of disease as will as for the identification of patients at risk for serious consequences. Once identified, these patients will be the focus of intensive measures, both preventative and therapeutic, aimed at arresting progressive liver damage.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program--Cooperative Agreements (U19)
Project #
5U19AI040034-03
Application #
6100102
Study Section
Project Start
1998-08-01
Project End
1999-07-31
Budget Start
1997-10-01
Budget End
1998-09-30
Support Year
3
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
Stanford University
Department
Type
DUNS #
800771545
City
Stanford
State
CA
Country
United States
Zip Code
94305

  Publications

White, Bethany; Madden, Annie; Hellard, Margaret et al. (2013) Increased hepatitis C virus vaccine clinical trial literacy following a brief intervention among people who inject drugs. Drug Alcohol Rev 32:419-25
Yee, Russell M; Lehil, Mandeep S; Rongey, Catherine et al. (2013) Impaired lymphocyte reactivity measured by immune function testing in untransplanted patients with cirrhosis. Clin Vaccine Immunol 20:526-9
Page, Kimberly; Osburn, William; Evans, Jennifer et al. (2013) Frequent longitudinal sampling of hepatitis C virus infection in injection drug users reveals intermittently detectable viremia and reinfection. Clin Infect Dis 56:405-13
Reyes-del Valle, Jorge; de la Fuente, Cynthia; Turner, Mallory A et al. (2012) Broadly neutralizing immune responses against hepatitis C virus induced by vectored measles viruses and a recombinant envelope protein booster. J Virol 86:11558-66
Asher, Alice; Lum, Paula J; Page, Kimberly (2012) Assessing candidacy for acute hepatitis C treatment among active young injection drug users: a case-series report. J Assoc Nurses AIDS Care 23:16-29
Dias, Paulo Telles; Hahn, Judith A; Delwart, Eric et al. (2011) Temporal changes in HCV genotype distribution in three different high risk populations in San Francisco, California. BMC Infect Dis 11:208
Bacchetti, Peter; Boylan, Ross; Astemborski, Jacquie et al. (2011) Progression of biopsy-measured liver fibrosis in untreated patients with hepatitis C infection: non-Markov multistate model analysis. PLoS One 6:e20104
Levy, Vivian; Evans, Jennifer L; Stein, Ellen S et al. (2010) Are young injection drug users ready and willing to participate in preventive HCV vaccine trials? Vaccine 28:5947-51
Diamond, Deborah L; Syder, Andrew J; Jacobs, Jon M et al. (2010) Temporal proteome and lipidome profiles reveal hepatitis C virus-associated reprogramming of hepatocellular metabolism and bioenergetics. PLoS Pathog 6:e1000719
Maher, Lisa; White, Bethany; Hellard, Margaret et al. (2010) Candidate hepatitis C vaccine trials and people who inject drugs: challenges and opportunities. Vaccine 28:7273-8

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