Abstract

Globally it is estimated that 71 million people have chronic hepatitis C, including 3 million in the United States. Virus transmission in the US increased sharply over the last decade amongst adolescents and young adults. As a consequence, the prevalence of maternal HCV infection doubled from 2009 to 2014. Diagnosis and treatment of these infections is uncommon. Little is known about the influence of pregnancy on chronic hepatitis C. We observed that about 50% of chronically infected women experience a sharp, spontaneous drop in viremia after childbirth. Observations from the last funding period implicate immunity in this post-partum control of persistent HCV replication. First, virus suppression was associated with HLA class II DP and IFNl3 genotype. Second, appearance of new escape mutations in class I HCV epitopes during postpartum virus suppression is consistent with recovery of exhausted antiviral CD8+ T cells. Third, declining viremia coincided with expansion of functional antiviral CD4+ T helper cells. This latter observation is significant because chronic hepatitis C outside of pregnancy is marked by stable viremia and an absence of circulating functional HCV-specific CD4+ T cells. The central hypothesis of this renewal application is that recovery of CD4+ T cell help results in restoration of CD8+ T cell and B cell responses that suppress HCV replication after childbirth.
Two specific aims are proposed.
Aim 1 will compare CD4+ (subaim 1a) and CD8+ (subaim 1b) T cell responses in women during and after pregnancy. We predict that recovered CD4+ T cells have phenotypic, transcriptional, and functional profiles consistent with T helper (Th) and T follicular helper (Tfh) sub-populations important for development of antiviral CD8+ T cells and B cells, respectively.
In Aim 1 b, we predict that virus suppression is associated with expansion of functional CD8+ T cells targeting intact class I HCV epitopes. CD8+ T cells targeting intact epitopes are the most thoroughly exhausted and difficult to rescue in chronic hepatitis C.
Aim 2 is to characterize HCV B cell responses in the unique setting of pregnancy. It will take advantage of an innovative tetramer comprised of the HCV E2 envelope glycoprotein to visualize and enrich antiviral B cells during and after pregnancy. This unique reagent will facilitate an analysis of whether B cells undergo changes in frequency, phenotype, transcriptional profile, and/or repertoire consistent with functional recovery and virus control. In parallel studies, whether antibody responses broaden after childbirth to neutralize contemporaneous viruses will be examined. In summary, these studies are expected to provide a detailed profile of T and B cell recovery during chronic infection, and insight into effector mechanisms relevant to development of a needed preventive HCV vaccine. More generally, we expect to fill an important gap in knowledge regarding persistent virus infections and immunity during pregnancy.

Public Health Relevance

Approximately 3 million people in the United States are chronically infected with the hepatitis C virus and are at increased risk for serious progressive liver diseases including liver cancer. Transmission of the virus has increased sharply in adolescents and young adults over the past 10 years. As a consequence, chronic hepatitis C has also become more common in women of childbearing age. The purpose of this research is to understand how immunity and persistent HCV replication are altered during pregnancy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
2R01AI096882-06
Application #
9597051
Study Section
Special Emphasis Panel (ZRG1)
Program Officer
Koshy, Rajen
Project Start
2012-02-01
Project End
2023-05-31
Budget Start
2018-06-18
Budget End
2019-05-31
Support Year
6
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
Nationwide Children's Hospital
Department
Type
DUNS #
147212963
City
Columbus
State
OH
Country
United States
Zip Code
43205

  Publications

Lanford, Robert E; Walker, Christopher M; Lemon, Stanley M (2017) The Chimpanzee Model of Viral Hepatitis: Advances in Understanding the Immune Response and Treatment of Viral Hepatitis. ILAR J 58:172-189
Walker, Christopher M (2017) Designing an HCV vaccine: a unique convergence of prevention and therapy? Curr Opin Virol 23:113-119
Ohmer, Samantha; Honegger, Jonathan (2016) New prospects for the treatment and prevention of hepatitis C in children. Curr Opin Pediatr 28:93-100
Honegger, Jonathan R; Tedesco, Dana; Kohout, Jennifer A et al. (2016) Influence of IFNL3 and HLA-DPB1 genotype on postpartum control of hepatitis C virus replication and T-cell recovery. Proc Natl Acad Sci U S A 113:10684-9
Price, Aryn A; Tedesco, Dana; Prasad, Mona R et al. (2016) Prolonged activation of innate antiviral gene signature after childbirth is determined by IFNL3 genotype. Proc Natl Acad Sci U S A 113:10678-83
Walker, Christopher M; Grakoui, Arash (2015) Hepatitis C virus: why do we need a vaccine to prevent a curable persistent infection? Curr Opin Immunol 35:137-43
Nelson, Chase W; Hughes, Austin L (2015) Within-host nucleotide diversity of virus populations: insights from next-generation sequencing. Infect Genet Evol 30:1-7
Price, Aryn A; Grakoui, Arash; Honegger, Jonathan R (2014) HCV adaptations to altered CD8(+) T-cell immunity during pregnancy. Future Virol 9:333-336
Honegger, Jonathan R; Zhou, Yan; Walker, Christopher M (2014) Will there be a vaccine to prevent HCV infection? Semin Liver Dis 34:79-88
Prasad, Mona R; Honegger, Jonathan R (2013) Hepatitis C virus in pregnancy. Am J Perinatol 30:149-59

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