Detection of a Broad Range of Low-Level Major Histocompatibility Complex Class II–Restricted, Hepatitis Delta Virus (HDV)–Specific T-Cell Responses Regardless of Clinical Status. (23rd September 2018)

Record Type:
Journal Article
Title:
Detection of a Broad Range of Low-Level Major Histocompatibility Complex Class II–Restricted, Hepatitis Delta Virus (HDV)–Specific T-Cell Responses Regardless of Clinical Status. (23rd September 2018)
Main Title:
Detection of a Broad Range of Low-Level Major Histocompatibility Complex Class II–Restricted, Hepatitis Delta Virus (HDV)–Specific T-Cell Responses Regardless of Clinical Status
Authors:
Landahl, Johanna
Bockmann, Jan Hendrik
Scheurich, Christoph
Ackermann, Christin
Matzat, Verena
Heide, Janna
Nuurei, Tungalag
D'Antonio, Gianluca
von Felden, Johann
Sette, Alessandro
Peine, Sven
Lohse, Ansgar W
Luetgehetmann, Marc
Marget, Matthias
Sidney, John
Schulze zur Wiesch, Julian
Abstract:
Abstract: Background: This study aimed to comprehensively define the breadth and specificity of the hepatitis delta virus (HDV)–specific T-cell response in patients at different stages of chronic coinfection with hepatitis B virus (HBV). Methods: Following in vitro stimulation with an overlapping set of 21 HDV-specific 20mer peptides and exogenous interleukin 2, HDV-specific CD4 + and CD8 + T-cell responses of 32 HDV-infected patients were analyzed by enzyme-linked immunospot analysis and intracellular cytokine staining for interferon γ production at the single-peptide level. Additionally, HLA-binding studies were performed both in silico and in vitro. Results: We were able to detect ≥1 T-cell response in >50% our patients. Interestingly, there was no significant difference between the breadth of the response in patients positive and those negative for HDV by PCR. HDV-specific T-cell responses focused on 3 distinct HDV-specific epitopes that were each detected in 12%–21% of patients—2 HLA class II–restricted epitopes (amino acids 11–30 and 41–60) and 1 major histocompatibility complex class I–restricted epitope (amino acids 191–210). In in vitro HLA-binding assays, the 2 CD4 + T-cell specificities (amino acids 11–30 and 41–60) showed promiscuous binding to multiple HLA-DR molecules. Conclusions: This comprehensive characterization of HDV T-cell epitopes provides important information that will facilitate further studies of HDV immunopathogenesis.
Is Part Of:
Journal of infectious diseases. Volume 219:Number 4(2019)
Journal:
Journal of infectious diseases
Issue:
Volume 219:Number 4(2019)
Issue Display:
Volume 219, Issue 4 (2019)
Year:
2019
Volume:
219
Issue:
4
Issue Sort Value:
2019-0219-0004-0000
Page Start:
568
Page End:
577
Publication Date:
2018-09-23
Subjects:
Hepatitis delta -- HDV -- CD4+ -- CD8+ -- T-cell epitope -- HLA binding
Communicable diseases -- Periodicals
Diseases -- Causes and theories of causation -- Periodicals
Medicine -- Periodicals
Communicable Diseases -- Periodicals
Electronic journals
616.9
Journal URLs:
http://jid.oxfordjournals.org/content/by/year
http://www.journals.uchicago.edu/JID/journal/
http://www.jstor.org/journals/00221899.html
http://ukcatalogue.oup.com/
DOI:
10.1093/infdis/jiy549
Languages:
English
ISSNs:
0022-1899
Deposit Type:
Legaldeposit
View Content:
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