Autoantibodies and Direct-acting Antivirals

University of Bari191 enrolled

Overview

The investigators assessed non-organ-specific antibodies before and 24 weeks after the end of therapy with direct-acting antivirals, in order to better clarify the clinical relevance of these antibodies in terms of treatment response and prognostic value. To achieve this goal patients with hepatitis C virus related advanced liver disease, with detectable circulating autoantibodies on at least two determinations before treatment, were enrolled.

About 40-70% of hepatitis C virus patients develop at least an autoimmune extra-hepatic disorder presumably due to the interaction between hepatitis C virus E2 envelope protein and B lymphocyte Cluster of Differentiation-81 receptor. In addition, the same interaction is responsible for the production of different serum non-organ-specific antibodies. The clinical significance of the latter phenomenon has not been fully understood except for the presence of liver kidney microsome-1 antibody, which is linked to a molecular mimicry between the cytochrome enzyme CYP2D6, primarily expressed in the liver, and hepatitis C virus proteins in genetically predisposed subjects. Actually, no data are available about the prevalence and clinical significance of serum non-organ-specific antibodies in hepatitis C virus patients treated with second generation direct-acting antivirals.

Study Type

OBSERVATIONAL

Enrollment

191

Conditions

Viral Hepatitis C Therapy Adverse Effect

Interventions

Non-organ-specific Ab positiveBIOLOGICAL

Antiviral administration and evaluation of SVR24 and side effects

Non-organ-specific Ab negativeBIOLOGICAL

direct-acting antiviral agents

Eligibility

Sex: ALLMin age: 18 Years

Medical Language ↔ Plain English

Inclusion Criteria: HCV positive patients Presence of advanced liver fibrosis Eligibility to the treatment with direct-acting antiviral therapy. Exclusion Criteria: History of autoimmune hepatitis and/or cholangitis Evidence of active hepatocellular carcinoma Human immunodeficiency virus coinfection Hepatitis B virus coinfection.

Locations (1)

Policlinic Hospital

Bari, Italy

Outcomes

Primary Outcomes

Sustained virological response

Evaluation of HCV-RNA levels

Time frame: 24 weeks after the end of antiviral therapy

Secondary Outcomes

Disappearance of non-organ-specific antibodies

Evaluation of anti nuclear antibodies, anti smooth muscle antibodies, liver kidney microsome antibodies

Time frame: 24 weeks after the end of antiviral therapy

Side effects

Clinical manifestations and laboratory alterations

Time frame: 24 weeks after the end of antiviral therapy

Data from ClinicalTrials.gov

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