Detail Article

Informations générales (source: ClinicalTrials.gov)

Numéro NCT

NCT03753308 Statut inconnu

Titre

Mechanism of DCs Dysfunction in Chronic HBV Infection (HepatoDC)

Type

Observational

Pathologie

Stéatose hépatique
Stéatose hépatique non alcoolique

Phase

Promoteur

University Hospital, Grenoble (Voir sur ClinicalTrials)

Date de début

décembre 2018

Date de fin

décembre 2022

Dernière mise à jour

29 juin 2024

Résumé

This research is to better understand the functional impairments of Dendritic cells (DCs) in chronic HBV infection. Aim is to determine if the virus is able to bind to the C-type lectin receptor (CLRs) of DCs to modulate their functions, also, to define the role of viral components and the molecular mechanisms of DCs modulation by HBV. This project should provide a better understanding of the mechanisms by which the immune response is altered by HBV and the immunological control of the infection, and thus propose new immunotherapeutic strategies based on the restoration of DC functions by releasing of virally-induced inhibitions, compromising the infection chronicity

Détail

Voir le détail Currently, chronic hepatitis B virus (HBV) infection therapies are limited to pegylated interferon alpha (Peg-IFNα) and nucleos(t)ide analogues (NUCs), alone or in combination. Even though they can reduce viremia level (circulating viral load), the loss of HBs antigen (HBsAg), which indicates functional clearance of the virus, is achieved in less than 10% of cases. The absence of curative treatment to eliminate the infection justifies the need to define new targets and to develop new therapeutic strategies, with an immuno-therapeutic component. Chronic HBV infection is associated with persistent and virally-induced immune deficiency. The immunological control of the infection seems essential to the functional clearance of the virus. The restoration of appropriate immune responses against the virus could prove to be a promising therapeutic strategy. However, the mechanisms in which HBV modulates immune function is still poorly understood. Dendritic cells (DCs) have an essential role in immunity. They play a central role in the induction and regulation of immune responses. Also, they play a particularly crucial role in the induction and orientation of antiviral immunity due to their unique properties at the interface between innate and acquired immune responses. In several chronic viral infections, DCs appear defective. The immune responses induced in the early stages of infection seem to be a crucial guide on the progression of the infection into the resolution or the chronicity. Objective of the investigators is to better understand the virus escape mechanism from immune control, particularly, to determine the mechanisms in which the virus modulates the functions of DCs, crucial for the subsequent orientation of antiviral immune responses, to define the molecular mechanisms of this inhibition and their consequences on the antiviral effectors functions, in order to propose new immunotherapeutic approaches that compromise the chronicity of the infection and treat the infection permanently and definitively. Lastly, the investigators have shown that there are functional impairments in plasmacytoid DCs (pDCs) in patients with chronic hepatitis B, associated with a lack of cytotoxic activity of NK cells. The Subverting of pDCs in HBV patients could be related to IP-10 and HBsAg and HBeAg antigens or other viral components (infectious particles or circulating HBcAg). In addition, HBV was able to inhibit the production of IFNα by pDCs from healthy individuals in response to TLR9 agonists, by the presence of inhibitory CpG sequences in its genome. This mechanism would allow the virus to actively escape the innate immune response mounted by pDCs. Recently, investigators have found an alteration of lectin C-type receptor (CLR) expression on pDCs of HBV patients compared to healthy donors as well as a phenotypic and functional modulation in the 3 major subtypes of DCs (mDCs BDCA1 +, pDCs BDCA2 + and mDCs BDCA3 +) in the context of chronic HBV infection. These major subversions of DCs, crucial cells for subsequent orientation of antiviral immune responses, support the hypothesis that HBV might deflect immunity by impacting these cells. In this clinical trial, investigators would like to pursue their research to better understand the functional impairments of DCs in chronic HBV infection, by defining if the virus is able to bind to the CLRs of DCs to modulate their functions, and by defining the role of viral components and the molecular mechanisms of DCs modulation by HBV. This project should provide a better understanding of the mechanisms of the immune response orientation by HBV and the immunological control of the infection, and thus propose new immunotherapeutic strategies based on the restoration of DC functions by releasing of virally-induced inhibitions, compromising the infection chronicity Fermer le détail

Etablissements

Les établissements hors Île-de-France dont les données sont issues de ClinicalTrials.gov Origine et niveau de fiabilité des données
Chu Grenoble Alpes - 38043 - Grenoble - France	Vincent LEROY	En recrutement		Contact (sur clinicalTrials)

Critères

Genre

Tous

Nombre d'inclusion

Critère d'inclusion

Inclusion Criteria :

Group 1a: HBV positive patients / no scheduled biopsy

- Surveyed as part of their usual care in Hepato-Gastroenterology clinic at CHUGA

- Patients who signed a non-opposition

- Patient affiliated to social security insurance

- HBsAg positive for more than 6 months

- known status of HBeAg (positive or negative)

- Treated or not with an antiviral

Group 1b: HBV positive patients / with scheduled biopsy

- Surveyed as part of their usual care in Hepato-Gastroenterology clinic at CHUGA

- Patients who signed a non-opposition

- Patient affiliated to social security insurance

- HBsAg positive for more than 6 months

- known status of HBeAg (positive or negative)

- Treated or not with an antiviral

- Patient with a liver biopsy indication as part of the treatment within 3 months.

Group 2: NASH patients / with scheduled biopsy

- Surveyed as part of their usual care in Hepato-Gastroenterology clinic at CHUGA

- Patients who signed a non-opposition

- Patient affiliated to social security insurance

- The existence of at least one element of metabolic syndrome

- Steatosis detected by non-invasive tests (echo, CAP, MRI)

Group 3: Blood samples from healthy donors

- No subject will be included in this group, the samples have been already collected
at EFS from healthy donors who had previously given their informed consents for
using their blood samples in the research.

- The blood samples have been collected in sufficient quantity to carry out the
analyzes (20mL from each donor).

Exclusion Criteria:

For groups 1a, 1b and 2 (HBV or NASH patients):

- Positive serology for HCV, HDV, HTLV, HIV

- Active autoimmune diseases

- Immunosuppressive therapies

- Cancer <2 years

- Alcohol: male> 30g / day, female> 20g / day

Group 1a and 1b:

- NASH patients

Group 2:

- Positive HBsAg Group 3: Blood samples from healthy donors

- Positive serology for HCV, HTLV, HIV, HBV (in the sense of a positive HBsAg test).

- Risk of any infectious disease at the time of sample collection (including fever> 38
° C over the past 15 days or recent contact with a person with a contagious
disease).

- Autoimmune disease or immunosuppressive therapy at the time of sample collection.

Critère de non inclusion

NCT03753308 - Mechanism of DCs Dysfunction in Chronic HBV Infection (HepatoDC)

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