Chronic hepatitis C infection blocks the ability of dendritic cells to secrete IFN-α and stimulate T-cell proliferation

Dendritic cells (DCs) are likely to play a key role in the compromised T‐cell function associated with hepatitis C Virus (HCV) infection. However, studies of DC function in HCV‐infected patients to date have yielded conflicting findings possibly because of patient and virus heterogeneity. Here, we r...

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Bibliographic Details
Published in:Journal of viral hepatitis 2011-12, Vol.18 (12), p.840-851
Main Authors: Ryan, E. J., Stevenson, N. J., Hegarty, J. E., O'Farrelly, C.
Format: Article
Language:English
Subjects:
Aged
alpha -Interferon
Antiviral agents
beta -Interferon
CD86 antigen
Cell Proliferation
Chronic infection
cytokines
dendritic cell
Dendritic cells
Dendritic Cells - immunology
Female
Genotypes
Hepatitis C
Hepatitis C virus
Hepatitis C, Chronic - immunology
Hepatitis C, Chronic - pathology
Humans
IFN-α
Immune Tolerance
Immunoglobulins
Interferon-alpha - secretion
Interleukin 8
Lipopolysaccharides
Liver diseases
Lymphocytes T
Male
Middle Aged
Mixed leukocyte reaction
Monocytes
Signal transduction
T-cell proliferation
T-Lymphocytes - immunology
TLR4 protein
toll-like receptor
Toll-like receptors
Vaccines
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Summary:Dendritic cells (DCs) are likely to play a key role in the compromised T‐cell function associated with hepatitis C Virus (HCV) infection. However, studies of DC function in HCV‐infected patients to date have yielded conflicting findings possibly because of patient and virus heterogeneity. Here, we report the characterization of monocyte‐derived DCs obtained from a homogenous cohort of women who were infected with HCV genotype 1b following exposure to contaminated anti‐D immunoglobulin from a single donor source. Patients included in the study had not received anti‐viral therapy and all had mild liver disease. We show that phenotypically normal monocyte‐derived dendritic cells (MDDCs) (CD11c+HLA−DR+CD1a+CD14lo) can be obtained from these patients. These cells respond to both Poly(I:C) and LPS, by up‐regulating expression of CD86. They secrete high levels of IL‐8 and CCL5 in response to LPS, an indication that the MyD88‐dependent and MyD88‐independent signalling pathways downstream of TLR4 ligation are functioning normally. However, these cells are poor stimulators of T‐cell proliferation in allogeneic mixed lymphocyte reactions. Furthermore, patient MDDCs fail to secrete IFN‐α in response to poly(I:C) or IFN‐β stimulation. Altered DC function may contribute to impaired cellular immune responses and chronicity of disease following HCV infection in this cohort. An effective therapeutic vaccine for chronic HCV infection will most likely need to target DCs to elicit an appropriate cellular response; therefore, it is important to resolve how the DCs of different patient cohorts respond to stimulation via TLRs.
ISSN:1352-0504
1365-2893
DOI:10.1111/j.1365-2893.2010.01384.x