Abstract
The E2 envelope glycoprotein of the hepatitis C virus (HCV) is a major target of broadly neutralizing antibodies that are closely related to a spontaneous cure of HCV infection. There is still no data about the diversity of E2-specific antibodies (Abs) glycosylation. The aim of this study was to analyze the level and sialylation of E2 IgG Abs, the relation of the respective changes to hepatic fibrosis (F) progression and their possible association with the efficacy of interferon-α-2a plus ribavirin (IFN-RBV) antiviral therapy. One hundred three HCV infected treatment-naive patients were examined using ELISA with E2 recombinant protein as antigen and sialic acid-specific Sambucus nigra agglutinin. The efficacy of the IFN-RBV treatment of patients with HCV dominant 1b and 3a genotypes (GT) was evaluated. A significant decrease of E2 Abs sialylation in the late stages of fibrosis was found irrespective of HCV genotype. On this basis, the F4 stage of fibrosis can be discriminated from its F0 or F1-3 stage by an about 75-79% accuracy. HCV infection of 1b genotype is associated with the production of lower sialylated E2 Abs, a higher frequency of F4 stage fibrosis, and a worse response to antiviral therapy. The increased SNA reactivity of E2 Abs was observed in patients with a sustained virological response (SVR). The proportion of SVR responders was significantly higher among patients with 3a genotype. However, for both dominant HCV genotypes (3a and 1b), an increased sialylation of E2 IgG was associated with a higher rate of patients with sustained virological response to antiviral therapy. Thus, the association of alterations of anti-E2 IgG Abs sialylation with hepatic fibrosis stage, HCV genotype, and the efficacy of antiviral therapy enables using these changes as novel noninvasive predictive biomarkers. The clinical potential of these findings is discussed.
Highlights
Hepatitis C virus (HCV) is a serious health problem worldwide and patients with this infection remain a difficult-tocure population [1, 2]
HCV envelope glycoproteins E1 and E2 play an important role in the HCV entry process, and the tetraspanin CD81 is the best-characterized entry factor which has been shown to interact with the HCV E2 envelope glycoprotein [3,4,5]
Compared to 1b GT, a significantly higher E2-specific Abs (E2 Abs) sialylation was detected in patients infected with HCV 3a genotype. For both dominant HCV genotypes (3a and 1b), an increased sialylation of E2 IgG was associated with a higher rate of patients with a sustained virological response (SVR) to antiviral therapy
Summary
Hepatitis C virus (HCV) is a serious health problem worldwide and patients with this infection remain a difficult-tocure population [1, 2]. The main aim of this investigation was to analyze the level and sialylation of E2 IgG Abs, the relation of the respective changes to hepatic fibrosis progression, and their possible impact on the efficacy of (IFN-RBV) antiviral therapy. A significant decrease of E2 Abs sialylation was observed in the late stages of fibrosis (F), irrespective of HCV genotype (GT), and viral load level. These changes showed a rather high level of sensitivity and specificity (above 75%).
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