Role of lymphatic system in the persistence and pathogenesis of woodchuck hepatitis virus infection

Thesis (Ph.D.)--Memorial University of Newfoundland, 2009. Medicine Includes bibliographical references (leaves 296-325) Hepatitis B virus (HBV) causes acute liver inflammation that apparently resolves completely or advances to chronic hepatitis, cirrhosis and hepatocellular carcinoma. These differe...

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Bibliographic Details
Main Author: Gujar, Shashi Ashok.
Other Authors: Memorial University of Newfoundland. Faculty of Medicine
Format: Thesis
Language:English
Published: 2008
Subjects:
Hepatitis B > Immunological aspects
Hepatitis B > Pathogenesis
Live > Lymphatics
Woodchuck > Virus diseases
Hepatitis B Virus
Woodchuck > immunology
Woodchuck > pathogenicity
T-Lymphocytes
Newfoundland studies
University of Newfoundland
Online Access:http://collections.mun.ca/cdm/ref/collection/theses4/id/161666
id ftmemorialunivdc:oai:collections.mun.ca:theses4/161666
record_format openpolar
spelling ftmemorialunivdc:oai:collections.mun.ca:theses4/161666 2023-05-15T17:23:34+02:00 Role of lymphatic system in the persistence and pathogenesis of woodchuck hepatitis virus infection Gujar, Shashi Ashok. Memorial University of Newfoundland. Faculty of Medicine 2008 xxi, 327 leaves : ill.(some col.) Image/jpeg; Application/pdf http://collections.mun.ca/cdm/ref/collection/theses4/id/161666 Eng eng Electronic Theses and Dissertations (39.59 MB) -- http://collections.mun.ca/PDFs/theses/Gujar_ShashiAshok.pdf a3241827 http://collections.mun.ca/cdm/ref/collection/theses4/id/161666 The author retains copyright ownership and moral rights in this thesis. Neither the thesis nor substantial extracts from it may be printed or otherwise reproduced without the author's permission. Paper copy kept in the Centre for Newfoundland Studies, Memorial University Libraries Hepatitis B--Immunological aspects Hepatitis B--Pathogenesis Live--Lymphatics Woodchuck--Virus diseases Hepatitis B Virus Woodchuck--immunology Woodchuck--pathogenicity T-Lymphocytes Text Electronic thesis or dissertation 2008 ftmemorialunivdc 2015-08-06T19:22:43Z Thesis (Ph.D.)--Memorial University of Newfoundland, 2009. Medicine Includes bibliographical references (leaves 296-325) Hepatitis B virus (HBV) causes acute liver inflammation that apparently resolves completely or advances to chronic hepatitis, cirrhosis and hepatocellular carcinoma. These differential outcomes of HBV infection are orchestrated to a large extent by the virus-specific T cell responses, which characteristically appear late after exposure to hepadnavirus. In this context, the objective of this study was to delineate the kinetics and understand inter-relationships between virus-specific and non-specific T cell proliferative, humoral as well as innate cytokine responses, along with serological and molecular markers of hepadnaviral infection induced after exposure and re-exposure to liver pathogenic or nonpathogenic doses of woodchuck hepatitis virus (WHV). Our results revealed that infection of woodchucks with either a liver pathogenic (>103 virions) or nonpathogenic (<103 virions) dose of WHV induced strong, but delayed, virus-specific T cell responses with comparable kinetics. Interestingly, immediately after exposure to virus, the non-specific proliferative capacity of lymphocytes in response to mitogenic stimulation was heightened and then subsided preceding the appearance of WHV-specific T cell response. This augmented non-specific proliferative reactivity was accompanied by the increased expression of interferon-alpha (IFN-α), interleukin-12 (IL-12) and IL-2 in circulating lymphoid cells; while its decline was associated with activation-induced cell death of lymphocytes. Importantly, the postponement of virus-specific T cell response coincided with the absence of TNF-α expression, while its rise was marked by synchronously elevated expression of TNF-α, IFN-α, IFN-γ, IL-2, IL-12, and IL-10 in lymphoid cells. Nonetheless, the virus-specific T cell responses induced during low-dose (occult) infection, in contrast to infection caused by liver pathogenic dose, did not provide protection against viral hepatitis. -- We conclude that hepadnavirus infections induce delayed virus-specific T cell proliferative responses irrespective of the dose of invading virus and symptomatic or asymptomatic outcome of the infection. This postponement of anti-viral T cell responses is preceded by the aberrant activation of lymphocyte and innate cytokine responses. Such an impaired activation of immune responses following hepadnavirus infection represents a possible mechanism that allows evasion of initial clearance and subsequent elimination of virus, permits its dissemination, and contributes to the establishment of persistence. Thesis Newfoundland studies University of Newfoundland Memorial University of Newfoundland: Digital Archives Initiative (DAI)
institution Open Polar
collection Memorial University of Newfoundland: Digital Archives Initiative (DAI)
op_collection_id ftmemorialunivdc
language English
topic Hepatitis B--Immunological aspects
Hepatitis B--Pathogenesis
Live--Lymphatics
Woodchuck--Virus diseases
Hepatitis B Virus
Woodchuck--immunology
Woodchuck--pathogenicity
T-Lymphocytes
spellingShingle Hepatitis B--Immunological aspects
Hepatitis B--Pathogenesis
Live--Lymphatics
Woodchuck--Virus diseases
Hepatitis B Virus
Woodchuck--immunology
Woodchuck--pathogenicity
T-Lymphocytes
Gujar, Shashi Ashok.
Role of lymphatic system in the persistence and pathogenesis of woodchuck hepatitis virus infection
topic_facet Hepatitis B--Immunological aspects
Hepatitis B--Pathogenesis
Live--Lymphatics
Woodchuck--Virus diseases
Hepatitis B Virus
Woodchuck--immunology
Woodchuck--pathogenicity
T-Lymphocytes
description Thesis (Ph.D.)--Memorial University of Newfoundland, 2009. Medicine Includes bibliographical references (leaves 296-325) Hepatitis B virus (HBV) causes acute liver inflammation that apparently resolves completely or advances to chronic hepatitis, cirrhosis and hepatocellular carcinoma. These differential outcomes of HBV infection are orchestrated to a large extent by the virus-specific T cell responses, which characteristically appear late after exposure to hepadnavirus. In this context, the objective of this study was to delineate the kinetics and understand inter-relationships between virus-specific and non-specific T cell proliferative, humoral as well as innate cytokine responses, along with serological and molecular markers of hepadnaviral infection induced after exposure and re-exposure to liver pathogenic or nonpathogenic doses of woodchuck hepatitis virus (WHV). Our results revealed that infection of woodchucks with either a liver pathogenic (>103 virions) or nonpathogenic (<103 virions) dose of WHV induced strong, but delayed, virus-specific T cell responses with comparable kinetics. Interestingly, immediately after exposure to virus, the non-specific proliferative capacity of lymphocytes in response to mitogenic stimulation was heightened and then subsided preceding the appearance of WHV-specific T cell response. This augmented non-specific proliferative reactivity was accompanied by the increased expression of interferon-alpha (IFN-α), interleukin-12 (IL-12) and IL-2 in circulating lymphoid cells; while its decline was associated with activation-induced cell death of lymphocytes. Importantly, the postponement of virus-specific T cell response coincided with the absence of TNF-α expression, while its rise was marked by synchronously elevated expression of TNF-α, IFN-α, IFN-γ, IL-2, IL-12, and IL-10 in lymphoid cells. Nonetheless, the virus-specific T cell responses induced during low-dose (occult) infection, in contrast to infection caused by liver pathogenic dose, did not provide protection against viral hepatitis. -- We conclude that hepadnavirus infections induce delayed virus-specific T cell proliferative responses irrespective of the dose of invading virus and symptomatic or asymptomatic outcome of the infection. This postponement of anti-viral T cell responses is preceded by the aberrant activation of lymphocyte and innate cytokine responses. Such an impaired activation of immune responses following hepadnavirus infection represents a possible mechanism that allows evasion of initial clearance and subsequent elimination of virus, permits its dissemination, and contributes to the establishment of persistence.
author2 Memorial University of Newfoundland. Faculty of Medicine
format Thesis
author Gujar, Shashi Ashok.
author_facet Gujar, Shashi Ashok.
author_sort Gujar, Shashi Ashok.
title Role of lymphatic system in the persistence and pathogenesis of woodchuck hepatitis virus infection
title_short Role of lymphatic system in the persistence and pathogenesis of woodchuck hepatitis virus infection
title_full Role of lymphatic system in the persistence and pathogenesis of woodchuck hepatitis virus infection
title_fullStr Role of lymphatic system in the persistence and pathogenesis of woodchuck hepatitis virus infection
title_full_unstemmed Role of lymphatic system in the persistence and pathogenesis of woodchuck hepatitis virus infection
title_sort role of lymphatic system in the persistence and pathogenesis of woodchuck hepatitis virus infection
publishDate 2008
url http://collections.mun.ca/cdm/ref/collection/theses4/id/161666
genre Newfoundland studies
University of Newfoundland
genre_facet Newfoundland studies
University of Newfoundland
op_source Paper copy kept in the Centre for Newfoundland Studies, Memorial University Libraries
op_relation Electronic Theses and Dissertations
(39.59 MB) -- http://collections.mun.ca/PDFs/theses/Gujar_ShashiAshok.pdf
a3241827
http://collections.mun.ca/cdm/ref/collection/theses4/id/161666
op_rights The author retains copyright ownership and moral rights in this thesis. Neither the thesis nor substantial extracts from it may be printed or otherwise reproduced without the author's permission.
_version_ 1766113341134077952

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