HCV-Induced Immune Responses Influence the Development of Operational Tolerance After Liver Transplantation in Humans

Bohne, Felix; Londoño, María-Carlota; Benítez, Carlos; Miquel, Rosa; Martínez‐Llordella, Marc; Russo, C; Ortíz, Cecilia; Bonaccorsi‐Riani, Eliano; Berthou, Christian; Bauer, Tanja; Protzer, Ulrike; Jaeckel, Elmar; Taubert, Richard; Forns, Xavier; Navasa, Miquel; Berenguer, Marina; Rimola, Antoni; Lozano, Juan José; Sánchez‐Fueyo, Alberto

doi:10.1126/scitranslmed.3008793

Cited by 76 publications

(95 citation statements)

References 48 publications

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“…A similar mechanism may be driven by CMV infection after LTx, which also causes inflammation in the graft and in other organs (52), whereas CMV is able to induce IFN-a production (56). A possible relationship between inflammation and reduced alloresponses after LTx is supported by a recent study that showed that chronic HCV patients who are operationally tolerant after LTx overexpress type I IFN and IFN-stimulated genes in the liver graft (57). A second possible explanation for the association between CMV infection and CD8 + T cell hyporesponsiveness is that CMV produces viral IL-10 (58), which inhibits the expansion of alloreactive CD8 + T cells.…”

Section: Discussionmentioning

confidence: 60%

Cytomegalovirus-Induced Expression of CD244 after Liver Transplantation Is Associated with CD8+ T Cell Hyporesponsiveness to Alloantigen

Mare-Bredemeijer

Shi

Mancham

et al. 2015

The Journal of Immunology

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The chronic presence of viral Ags can induce T cell exhaustion, which is characterized by upregulation of coinhibitory receptors and loss of T cell function. We studied whether a similar phenomenon occurs after liver transplantation (LTx), when there is continuous exposure to alloantigen. Expression of coinhibitory receptors on circulating CD4+ and CD8+ T cells was analyzed longitudinally in 19 patients until 6 mo after LTx and cross-sectionally in 38 patients late (1–12 y) after LTx. Expression of the coinhibitory receptors CD160 and CD244 on circulating CD8+ T cells was already higher 6 mo after LTx compared with pre-LTx, and the elevated expression was sustained late after LTx, with CD244 showing the more prominent increase. The strongest upregulation of CD244 on circulating CD8+ T cells was observed in patients who experienced CMV infection after LTx. CMV infection also was associated with reduced CD8+ T cell proliferation and cytotoxic degranulation in response to alloantigen late after LTx. Purified CD244+CD8+ T cells from LTx patients showed lower proliferative responses to alloantigen, as well as to polyclonal stimulation, than did their CD244− counterparts. In addition, the CD244+CD8+ T cell population contained the majority of CMV peptide–loaded MHC class I tetramer-binding cells. In conclusion, CMV infection after LTx, rather than persistence of alloantigen, induces the accumulation of dysfunctional CD244+CD8+ T cells in the circulation that persist long-term, resulting in reduced frequencies of circulating alloreactive CD8+ T cells. These results suggest that CMV infection restrains CD8+ T cell alloresponses after LTx.

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Section: Discussionmentioning

confidence: 60%

Cytomegalovirus-Induced Expression of CD244 after Liver Transplantation Is Associated with CD8+ T Cell Hyporesponsiveness to Alloantigen

Mare-Bredemeijer

Shi

Mancham

et al. 2015

The Journal of Immunology

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“…Interestingly, HCV infection does not negatively influence the establishment of operational tolerance of the liver allograft after the withdrawal of immunosuppression, whereas concomitant infections are generally considered to be detrimental to the process of allograft tolerance [62]. As expected, the induction of Treg might be involved in this phenomenon, alongside high levels of intrahepatic interferon-stimulated gene expression which may paradoxically promote a tolerogenic micro-environment in the context of HCV infection.…”

Section: Open Issues and Future Perspectivesmentioning

confidence: 81%

Role of regulatory T-cells during hepatitis C infection: From the acute phase to post-transplantation recurrence

Barjon

Dahlqvist

Calmus

et al. 2015

Digestive and Liver Disease

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Hepatitis C viral infection persists and becomes chronic in a majority of affected individuals. Numerous factors have been described to explain how the virus manages to escape the host immune system. One important escape mechanism is the increase in regulatory T cells induced by the virus. In this review, we will focus on the status of regulatory T cells throughout the natural history of hepatitis C infection and after liver transplantation. The molecular mechanisms involved in increasing the number of regulatory T cells are also discussed, as are data regarding the impact of regulatory T-cells on hepatic fibrosis in the context of hepatitis C viral infection.

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“…18,19 Based on these experimental observations, Alberto Sanchez-Fueyo and co-workers (London, UK) have demonstrated that persistent hepatitis C virus (HCV) infections exert clinical immunoregulatory effects that alleviate deleterious alloimmune responses. 20 This original work challenges the notion that heterologous immunity and inflammatory responses within the transplant will necessarily prevent tolerance.…”

Section: Deciphering Anti-infectious Immune Responses and Pathogen-inmentioning

confidence: 96%

Infectious Diseases in Transplantation—Report of the 20th Nantes Actualités Transplantation Meeting

Haspot

Halary²

2015

Transplantation

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The 20th Nantes Actualités Transplantation (NAT) meeting was held on June 11, 2015, and June 12, 2015. This year, the local organizing committee selected an update on infectious diseases in solid organ and hematopoietic stem cell transplantation. With an attendance of close to 170 clinicians, researchers, students, engineers, technicians, invited speakers, and guests from North and South America, Germany, Switzerland, Netherlands, and France, the meeting was well attended. Invited speakers' expertise covered basic as well as translational microbiology, immunology, transplantation, and intensive care medicine. This report identifies a number of advances presented during the meeting in the care and management of infectious diseases in transplantation and immunocompromised patients. New antiviral immune responses and their modulation by pathogens in addition to novel antimicrobial therapeutic strategies, cell therapies, and genomic analysis were discussed.

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HCV-Induced Immune Responses Influence the Development of Operational Tolerance After Liver Transplantation in Humans

Cited by 76 publications

References 48 publications

Cytomegalovirus-Induced Expression of CD244 after Liver Transplantation Is Associated with CD8+ T Cell Hyporesponsiveness to Alloantigen

Cytomegalovirus-Induced Expression of CD244 after Liver Transplantation Is Associated with CD8+ T Cell Hyporesponsiveness to Alloantigen

Role of regulatory T-cells during hepatitis C infection: From the acute phase to post-transplantation recurrence

Infectious Diseases in Transplantation—Report of the 20th Nantes Actualités Transplantation Meeting

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