Abstract

Hepatitis E virus (HEV) infects >20 million people worldwide annually leading to >44,000 deaths due to HEV-related hepatobiliary diseases. A unique feature of HEV infection is fulminant hepatitis with high mortality of >25% in pregnant women. Due to the lack of an animal model, the underlying mechanism in the pathogenesis of HEV-associated fulminant hepatitis during pregnancy is unknown. The elevated levels of sex hormones such as progesterone and estrogen during pregnancy are known to promote certain virus replications including HEV. Accumulating evidence indicate that HEV replication is sex hormone-dependent, as HEV replication was significantly enhanced in the presence of sex hormones or pregnancy sera in infected cells. The recent discovery of HEV from rabbits led to the development of a pregnancy model for HEV, as fulminant hepatitis with high mortality was convincingly and independently reproduced in HEV-infected pregnant rabbits. The long-term goal is to identify the host (hormonal and immunological) and viral factors contributing to HEV-associated fulminant hepatic failure.
In aim 1, we will determine the effect and mechanism of pregnancy-associated sex hormones on HEV replication in human liver cells. We hypothesize that HEV infection inhibits the expression of estrogen receptor ER-? and ER-? during pregnancy, which results in suppression of host innate immunity leading to enhanced HEV replication. The effect of E1, E2 and P4, singly or in combination, on HEV replication in liver cells will be determined, and the underlying mechanisms of sex hormones in regulating HEV replication through the expression of estrogen receptor ER-?/ER-?, and progesterone receptor PGRMC1/PGRMC2 and their effect on cytokine expressions will be delineated.
In aim 2, we will elucidate the role and mechanism of pregnancy-associated sex hormones in the development of fulminant hepatitis using a rabbit model. We hypothesize that changes of pregnancy-associated sex hormones suppress host innate and cell-mediated immune responses leading to enhanced HEV replication and fulminant hepatitis. Pregnant rabbits will be infected with HEV to identify the sex hormones and immunological correlates in the development of fulminant hepatitis during pregnancy. The mechanisms of P4- and E1/E2-mediated fulminant hepatitis will be delineated by quantifying mRNA and protein expression levels of ER-?/ER-?, PGRMC1/PGRMC2, and progesterone-induced blocking factor in liver and placenta tissues, and their effect on cytokine expressions in infected rabbits.
In aim 3, we will define the viral genetic element(s) associated with fulminant hepatic failure. From case studies, 8 unique amino acid residues within HEV ORF1 are associated with fulminant hepatic failure. We hypothesize that these mutations significantly enhance HEV replication leading to higher viral loads and fulminant hepatic failure. We will first utilize HEV luciferase replicons to determine the effect of the 8 amino acid mutations on HEV replication in liver cells. The top 2 mutations with greatest enhancement on HEV replication will be introduced, singly and in combination, into genotype 3 HEV infectious clones to rescue mutant viruses, which will be used to infect pregnant rabbits to determine whether the identified mutations contribute to fulminant hepatitis. We anticipate to identify the sex hormone(s), underlying mechanisms, immunological correlates, and viral genetic element(s) contributing to the development of fulminant hepatic failure during HEV infection.

Public Health Relevance

Hepatitis E virus (HEV) infection causes fulminant hepatitis with high mortality rate of up to 25% in pregnant women but the underlying mechanisms are unknown. By using a pregnant rabbit HEV model and an in vitro HEV cell culture system, we will delineate the role and mechanisms of pregnancy-associated sex hormones in the development of fulminant hepatic failure during pregnancy. The information gained from this project will have important implications for devising effective strategies for the prevention and treatment of HEV-associated fulminant hepatic failure in pregnant women.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
2R01AI050611-14
Application #
9788856
Study Section
Hepatobiliary Pathophysiology Study Section (HBPP)
Program Officer
Koshy, Rajen
Project Start
2002-06-15
Project End
2024-04-30
Budget Start
2019-05-15
Budget End
2020-04-30
Support Year
14
Fiscal Year
2019
Total Cost
Indirect Cost

  Institution

Name
Virginia Polytechnic Institute and State University
Department
Veterinary Sciences
Type
Schools of Veterinary Medicine
DUNS #
003137015
City
Blacksburg
State
VA
Country
United States
Zip Code
24061

  Publications

Yugo, Danielle M; Cossaboom, Caitlin M; Heffron, Connie Lynn et al. (2018) Evidence for an unknown agent antigenically related to the hepatitis E virus in dairy cows in the United States. J Med Virol :
Yugo, Danielle M; Heffron, C Lynn; Ryu, Junghyun et al. (2018) Infection Dynamics of Hepatitis E Virus in Wild-Type and Immunoglobulin Heavy Chain Knockout JH-/- Gnotobiotic Piglets. J Virol 92:
Cao, Dianjun; Ni, Yan-Yan; Walker, Michelle et al. (2018) Roles of the genomic sequence surrounding the stem-loop structure in the junction region including the 3' terminus of open reading frame 1 in hepatitis E virus replication. J Med Virol 90:1524-1531
Cao, Dianjun; Ni, Yan-Yan; Meng, Xiang-Jin (2018) Substitution of amino acid residue V1213 in the helicase domain of the genotype 3 hepatitis E virus reduces virus replication. Virol J 15:32
Sooryanarain, Harini; Meng, Xiang-Jin (2018) Hepatitis E virus: reasons for emergence in humans. Curr Opin Virol 34:10-17
Sooryanarain, Harini; Rogers, Adam J; Cao, Dianjun et al. (2017) ISG15 Modulates Type I Interferon Signaling and the Antiviral Response during Hepatitis E Virus Replication. J Virol 91:
Cao, Dianjun; Cao, Qian M; Subramaniam, Sakthivel et al. (2017) Pig model mimicking chronic hepatitis E virus infection in immunocompromised patients to assess immune correlates during chronicity. Proc Natl Acad Sci U S A 114:6914-6923
Schwartzman, Julia A; Ruby, Edward G (2016) Stress as a Normal Cue in the Symbiotic Environment. Trends Microbiol 24:414-424
Yugo, Danielle M; Hauck, Ruediger; Shivaprasad, H L et al. (2016) Hepatitis Virus Infections in Poultry. Avian Dis 60:576-88
Cossaboom, Caitlin M; Heffron, Connie L; Cao, Dianjun et al. (2016) Risk factors and sources of foodborne hepatitis E virus infection in the United States. J Med Virol 88:1641-5

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