Evaluation of third-generation screening and confirmatory assays for HCV antibodies

• Published in: Vox sanguinis Vol. 66; no. 2; p. 122
• Main Authors: Uyttendaele, S, Claeys, H, Mertens, W, Verhaert, H, Vermylen, C
• Format: Journal Article
• Language: English
• Published: England 01.02.1994
• Subjects: Antigens, Viral - immunology; Blood Donors; Capsid - immunology; Cohort Studies; False Positive Reactions; Hepacivirus - immunology; Hepacivirus - isolation & purification; Hepatitis Antibodies - blood; Hepatitis C - epidemiology; Hepatitis C - prevention & control; Hepatitis C - transmission; Hepatitis C Antibodies; Hepatitis C Antigens; Humans; Immunoblotting; Immunoenzyme Techniques; Mass Screening - methods; Peptide Fragments - chemical synthesis; Peptide Fragments - immunology; Pilot Projects; Polymerase Chain Reaction; Recombinant Proteins - immunology; Renal Dialysis; Sensitivity and Specificity; Viral Nonstructural Proteins - immunology; Viremia - microbiology
• ISSN: 0042-9007; 1423-0410
• DOI: 10.1111/j.1423-0410.1994.tb00293.x

A third-generation (gen.) screening and immunoblot assay (Ortho EIA-3.0; Chiron RIBA-3 prototype), using antigens derived from the capsid and different nonstructural regions (NS3, NS4 and NS5) of the hepatitis C virus viral genome, were evaluated in comparison with the corresponding second-gen. assays (Ortho EIA-2.0; revised Ortho EIA-2.5; Chiron RIBA-2). In 203 depository sera of blood donors, positive in EIA-2.0, specificity of the screening assays was improved as shown by an increase in positive predictive value for viral carrier state from 0.23 (EIA-2.0) to 0.37 (EIA-2.5) and 0.52 (EIA-3.0). Comparing the confirmation patterns on RIBA-2 and RIBA-3, this amelioration was mainly due to the specific elimination of false-positive c22-3 and c100-3 reactions. Antibody response to the newly added NS5 antigen was not as prevalent as to the other antigens and had only a minor influence in sample allocation. In contrast, screening of 1,560 volunteer blood donors and 47 hemodialysis patients revealed 3 additional positive sera, only reacting with the NS5 antigen. However none of these isolated NS5 reactions could be confirmed on synthetic peptides [INNO-LIA: NS5(p)] and none was PCR positive. A documented seroconversion, detected earlier with EIA-3.0, was related to a better immunological response to the NS3 antigen and not to the additional NS5. From this pilot study third-gen. assays appeared extremely useful in the reevaluation of HCV-seropositive depository sera. However the additional value of the NS5 antigen in blood donor screening is still hypothetical and remains to be established in larger screening studies.