In vitro use of autologous dendritic cells improves detection of T cell responses to hepatitis B virus (HBV) antigens

Carotenuto, P; Artsen, Andrè; Niesters, Hubert G. M.; Osterhaus, Albert D. M. E.; Pontesilli, O.

doi:10.1002/jmv.21333

Cited by 17 publications

(14 citation statements)

References 33 publications

(35 reference statements)

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“…17 Similarly, other studies have shown that autologous moDCs loaded with recombinant HBV antigens were capable of stimulating autologous T-cell proliferation. [37][38][39] Because of their stimulatory capacity, moDCs loaded with recombinant antigens or synthetic peptides have been administered to patients in two clinical trials. In both cases, a significant improvement in virological parameters was observed in approximately 50% of the patients, with the HBeAg-negative patients responding best.…”

Section: Potential Of Modc Vaccinesmentioning

confidence: 99%

Dissecting the dendritic cell controversy in chronic hepatitis B virus infection

Gehring

D’Angelo

2014

Cell Mol Immunol

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Therapeutic vaccines to boost endogenous T-cell immunity rely on the stimulatory capacity of dendritic cells (DCs). The functionality of DCs in chronic hepatitis B virus (HBV) infection has been a long-standing debate. Therefore, we have attempted to summarize multiple studies investigating DC function in chronic HBV patients to determine whether common observations can be drawn. We found that the frequency and function of ex vivo-tested myeloid and plasmacytoid DCs were largely intact in patients with HBV infection and similar to those of healthy donor DCs. The main exception was reduced IFN-a production by plasmacytoid DC from chronic HBV patients. This reduced IFN-a production correlated with liver inflammation in multiple studies but not with viral load, suggesting that viral antigens have little effect on DC function. The majority of the confusion about DC function arises from studies reporting the reduced function of healthy donor DCs exposed to various sources of HBV in vitro. These direct effects of viral antigens are in contrast to data from HBV-infected patients. The variations in the assays used and areas that require further investigation are also covered

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Section: Potential Of Modc Vaccinesmentioning

confidence: 99%

Dissecting the dendritic cell controversy in chronic hepatitis B virus infection

Gehring

D’Angelo

2014

Cell Mol Immunol

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“…This strategy may be extended to other persistent infections and potentially open new avenues for immunotherapy. Currently, in vitrocultured moDCs loaded with recombinant antigens have been used to vaccinate patients with chronic HBV (47,48), HCV (49), and HIV (50-52) infection. These vaccines can enhance virus-specific T cell responses, but are hindered by the need to select appropriate antigens and a GMP cell production facility to produce the vaccine.…”

Section: Figurementioning

confidence: 99%

Mobilizing monocytes to cross-present circulating viral antigen in chronic infection

Gehring

Haniffa²,

Kennedy³

et al. 2013

J. Clin. Invest.

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Selection of antigens for therapeutic vaccination against chronic viral infections is complicated by pathogen genetic variations. We tested whether antigens present during persistent viral infections could provide a personalized antigenic reservoir for therapeutic T cell expansion in humans. We focused our study on the HBV surface antigen (HBsAg), which is present in microgram quantities in the serum of chronic HBV patients. We demonstrated by quantitative fluorescent microscopy that, out of 6 professional APC populations in the circulation, only CD14 monocytes (MNs) retained an HBsAg depot. Using TCR-redirected CD8 + T cells specific for MHC-I-restricted HBV epitopes, we showed that, despite being constantly exposed to antigen, ex vivoisolated APCs did not constitutively activate HBV-specific CD8 + T cells. However, differentiation of HBsAg + CD14 MNs from chronic patients to MN-derived DCs (moDCs) induced cross-presentation of the intracellular reservoir of viral antigen. We exploited this mechanism to cross-present circulating viral antigen and showed that moDCs from chronically infected patients stimulated expansion of autologous HBV-specific T cells. Thus, these data demonstrate that circulating viral antigen produced during chronic infection can serve as a personalized antigenic reservoir to activate virus-specific T cells. IntroductionTherapeutic vaccination for chronic infections, be it recombinant antigens, peptides, viral vectors, DNA, or DCs, are hindered by the need to select appropriate antigens. It is a major complicating factor due to the evolutionary diversity that pathogens have developed in response to selective forces exerted by individual (immune response) or environmental (drugs, vectors) factors. Moreover, peptides covering conserved regions for vaccination are HLA restricted and can only be applied to selected patients with the appropriate HLA. As a result, recombinant antigens or DNA vectors coding pathogen proteins may misdirect the intended immune response due to differences between the infectious pathogen and the antigen sequence utilized for vaccination.A hallmark of many chronic infections is the constant production of pathogen proteins. This is particularly evident in HBV infection, where viral titers can reach 10 9 -10 10 virions/ml in the serum. The HBV surface antigen (HBsAg) is produced in excess of whole virions and reaches concentrations well into the μg/ml range (1). While persistently present viral antigen is generally considered a negative factor (2), the abundance of endogenously produced viral antigen could be internalized by different cell types. Proper activation of cells internalizing antigen in the circulation of chronic patients could provide a target for therapeutic vaccination and stimulate T cells with antigen customized to the patient's viral genome.HBV does not infect or productively replicate in human PBMCs (3), and systematic analysis of cells capable of internalizing circu-

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“…In consideration of its immunomodulatory potential [4], IFN-a is predicted to act rapidly on HBV-specific T-cell responses since the effect on the immune system is direct rather than only indirectly mediated by the decline of viremia and antigenemia. However, little is known about the behavior of protective antiviral T-cells during the early phases of IFN therapy in e antigen (HBeAg)-negative genotype D chronic hepatitis B, since most published studies [5][6][7][8][9][10] have been focused on HBeAg-positive patients, who can have a different immunological reactivity to IFN, and have been conducted with a limited set of immunological assays, which can be inadequate to characterize thoroughly the IFN effect. Therefore, our study was done on a homogeneous group of HBeAg-negative genotype D CHB patients with positive baseline predictors of response to IFN, who should also have maximal probability of immunological improvement during therapy, using a comprehensive set of immunological parameters to avoid the risk of missing some effects of IFN therapy on T-cells.…”

Section: Introductionmentioning

confidence: 99%

Peginterferon-α does not improve early peripheral blood HBV-specific T-cell responses in HBeAg-negative chronic hepatitis

Penna

Laccabue

Libri

et al. 2012

Journal of Hepatology

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In vitro use of autologous dendritic cells improves detection of T cell responses to hepatitis B virus (HBV) antigens

Cited by 17 publications

References 33 publications

Dissecting the dendritic cell controversy in chronic hepatitis B virus infection

Dissecting the dendritic cell controversy in chronic hepatitis B virus infection

Mobilizing monocytes to cross-present circulating viral antigen in chronic infection

Peginterferon-α does not improve early peripheral blood HBV-specific T-cell responses in HBeAg-negative chronic hepatitis

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