Endogenous intrahepatic IFNs and association with IFN-free HCV treatment outcome

Meissner, Eric G.; Wu, David; Osinusi, Anu; Bon, Dimitra; Virtaneva, Kimmo; Sturdevant, Dan E.; Porcella, Steve; Wang, Honghui; Herrmann, Eva; McHutchison, John G.; Suffredini, Anthony F.; Polis, Michael A.; Hewitt, Stephen M.; Prokunina‐Olsson, Ludmila; Masur, Henry; Fauci, Anthony S.; Kottilil, Shyamasundaran

doi:10.1172/jci75938

Cited by 187 publications

(222 citation statements)

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“…As type I IFN has been shown to negatively control pDC numbers in various in vitro infection models, it was thus suggested that type I IFN might negatively regulate pDC numbers during HCV infection. A recent immunohistochemistry analysis in fact failed to detect any pDCs both in pretreatment and end-of-treatment human liver biopsies [40]. …”

Section: Induction Of Ifns and Isgs In Chronic Hcv Infection: The LIVmentioning

confidence: 99%

Activation of Type I and Type III Interferons in Chronic Hepatitis C

Mihm

2015

J Innate Immun

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Infection with hepatitis C virus (HCV) results in chronic and progressive liver disease. Persistency rates add up to 85%. Despite recognition of the virus by the human host in peripheral blood and in the liver, immune response appears to be ineffective in clearing infection. The ability to spontaneously eradicate the virus as well as the outcome of infection upon therapy with human recombinant interferon-α (IFN-α) was found to correlate most closely with genetic variations within the region encoding the IFN-λ genes, as revealed by genome-wide association studies on main ethnic populations in 2009. This review summarizes the induction of type I and type III IFN genes and their effectors, the IFN-stimulated genes. It focusses on the in vivo situation in chronic HCV infection in man both in the peripheral blood compartment and in the liver. It also addresses the impact of genetic polymorphisms in the region of type III IFN genes on their activation. Finally, it discusses how antiviral drugs (i.e. IFN-α, ribavirin and the direct-acting antivirals) may complementarily control the activation of endogenous IFNs and succeed in combatting infections.

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Section: Induction Of Ifns and Isgs In Chronic Hcv Infection: The LIVmentioning

confidence: 99%

Activation of Type I and Type III Interferons in Chronic Hepatitis C

Mihm

2015

J Innate Immun

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“…Similar studies showed that the rapid decline of HCV viral load by DAAs was associated with restored HCV specific memory T cell dedifferentiation, lymphocyte deactivation and normalized natural killer cell function [42][43][44]. Mir-122, which plays a central role in orchestrating hepatocarcinogenesis was recently found to be decreased in serum samples after IFN-free therapy [45]. IFN-free therapy leads to the downregulation of type II and III IFNs, their receptors and IFN stimulated genes [46].…”

Section: Molecular Mechanisms Of Hcc Occurrence or Recurrence With Damentioning

confidence: 84%

Hepatocellular Carcinoma Occurrence and Recurrence after Antiviral Treatment in HCV-Related Cirrhosis. Are Outcomes Different after Direct Antiviral Agents? A Review

Spârchez

Mocan²

2017

JGLD

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Hepatitis C virus (HCV) infection is one of the major causes of hepatocellular carcinoma (HCC) worldwide. In the last decades, several studies have showed a lower rate of HCC occurrence or recurrence in patients with HCV-related cirrhosis after interferon-based antiviral therapies compared to untreated controls, even without reaching viral clearance. Unfortunately, interferon regimens could only yield viral clearance in approximately half of the patients. The recent development of new all-oral regimens with direct-acting antivirals (DAAs) has radically improved the cure rate to above 90%. In respect to these findings, many would have thought that interferon-free regimens would decrease the development and recurrence of HCC. Literature data have unexpectedly reported high rates of both the occurrence and recurrence of HCC after therapy with DAAs. However, it is probably too early to express some concerns. More recent data showed that both occurrence and recurrence of HCC are decreased by the DAAs. Interferon-free therapy is definitely not without limits. Together with the initial thoughts of an increased risk of HCC, these may lead to an unwanted restricted access to interferon-free regimens in specific subpopulations. This issue should be settled as soon as possible because millions of hepatitis C patients are and will be using DAAs in the present and future. Our purpose is to review the existing literature and to offer a more precise and rational interpretation of the existing data.Key words: – – e – .Abreviations: AFP: alpha-fetoprotein; DAA: direct antiviral agent; HCC: hepatocellular carcinoma; HCV: hepatitis C virus; HR: hazard ratio; IFN: interferon; LDV: Ledispavir; SMV: Simeprevir; SOF: Sofosbuvir; SVR: sustained virologic response.

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“…HLA-A*0201-restricted HCC-specific peptides of AFP [137][138][139][140][141][142][143][144][145] (PLFQVPEPV), NY-ESO-1 157-165 (SLLMWITQC), MAGE-A3 112-120 (KVAELVHFL), MAGE-A10 [254][255][256][257][258][259][260][261][262] (GLYDGMEHL), SSX-2 [41][42][43][44][45][46][47][48][49] (KASEKIFYV) and p53 [149][150][151][152][153][154][155][156][157] (STPPPGTRV) at purities ranging from 82.78 to 97.99% were also obtained from ProImmune Ltd. For these HCC-associated epitope-specific peptides, corresponding PE-labeled MHC class I dextramers were obtained from Immudex (Copenhagen, Denmark). Further, HBV-specific 15-mer overlapping peptides covering the core (4 pools from 41 peptides) and polymerase regions (8 pools from 165 peptides) were purchased from ProImmune Ltd. Also, HLA-A*0201-restricted HBV-specific peptides Core [18][19][20][21][22][23][24][25][26][27] (FLPSDFFPSV), Env [183][184][185][186][187][188]…”

Section: Peptides Hla Class I Multimers and Recombinant Proteinsmentioning

confidence: 99%

“…PBMC from cirrh-to-No HCC patients (n = 17) isolated at TS, EOT, and FU were stimulated with the specific peptides in vitro. HBVspecific Core [18][19][20][21][22][23][24][25][26][27] , Env [183][184][185][186][187][188][189][190][191] , Pol 578-581 , and Surf 185-194 control peptide stimulations were used in selected patients with no HBV coinfection to secure the quality of staining (see online suppl. Fig 7).…”

Section: The Strength Of Hcc Epitope-specific Cd8+ T Cell Responses Dmentioning

confidence: 99%

“…For HCC arising from underlying cirrhosis in the context of therapy-induced HCV clearance, it is not known whether this is the case. Some recent studies suggest that IFN-free DAA therapy may alter the concentration of soluble inflammatory mediators (SIM) [18] and may evoke immune reconstitution of intrahepatic interferon-stimulated genes [19]. Whether or not such immunological changes influence the prevailing T cell immune surveillance machinery of HCC is still unclear.…”

Section: Introductionmentioning

confidence: 99%

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HCC Immune Surveillance and Antiviral Therapy of Hepatitis C Virus Infection

et al. 2018

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Objective: HCV clearance by current antiviral therapies improves clinical outcomes but falls short in eliminating the risk for hepatocellular carcinoma (HCC) emergence. As the HCC immune surveillance establishment is vital for the control of neoplastic development and growth, we investigated its correlation with on-/post-treatment HCC emergence, and further analyzed the influence of viral eradication on this setup in patients with HCV-related liver cirrhosis. Design: PBMC isolated at baseline and longitudinally during therapy were analyzed for tumorassociated antigen (TAA)-specific CD8+ T cell responses against glypican-3 overlapping peptides in vitro using high-definition flow cytometry. Multianalyte profiling of fifty soluble inflammatory mediators (SIM) in the plasma was also performed using Luminex-based multiplex technology. Results: Cirrhosis patients were characterized by an altered profile of distinct SIMs at baseline. At this time point, immune-surveilling T cells targeting specific HCC-associated antigens were readily detectable in HCV-free cirrhosis patients whilst being rather weak in such patients who further developed HCC upon virus eradication. Therapy-induced cure of HCV infection analogously reduced the strength of the prevailing HCC immune surveillance machinery, particularly by CD8+ T cells in cirrhosis patients. These results were further vali- dated by T cell reactivities to six immuno-dominant HCC-associated HLA-A2-restricted epitopes. Further, we demonstrated that this phenomenon was likely orchestrated by alterations in SIMs -with evidence of IL-12 being a major culprit. Conclusion: Given the relationship between the baseline HCC-specific immune surveilling T cell responses and therapy-associated HCC emergence, and the impact of HCV clearance on its strength and magnitude, we recommend a continued HCC screening in cirrhotic HCV patients despite HCV resolution.

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Endogenous intrahepatic IFNs and association with IFN-free HCV treatment outcome

Cited by 187 publications

References 50 publications

Activation of Type I and Type III Interferons in Chronic Hepatitis C

Activation of Type I and Type III Interferons in Chronic Hepatitis C

Hepatocellular Carcinoma Occurrence and Recurrence after Antiviral Treatment in HCV-Related Cirrhosis. Are Outcomes Different after Direct Antiviral Agents? A Review

HCC Immune Surveillance and Antiviral Therapy of Hepatitis C Virus Infection

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