Performance of Bio-Rad and Limiting Antigen Avidity Assays in Detecting Recent HIV Infections Using the Quebec Primary HIV-1 Infection Cohort

• Published in: PloS one Vol. 11; no. 5; p. e0156023
• Main Authors: Serhir, Bouchra, Hamel, Denis, Doualla-Bell, Florence, Routy, Jean Pierre, Beaulac, Sylvie-Nancy, Legault, Mario, Fauvel, Micheline, Tremblay, Cécile
• Format: Journal Article
• Language: English
• Published: United States Public Library of Science 25.05.2016; Public Library of Science (PLoS)
• Subjects: Acquired immune deficiency syndrome; Adult; AIDS; Algorithms; Analysis; Antigens; Antigens, Viral - blood; Antiretroviral drugs; Assaying; Avidity; Biology and Life Sciences; Biomarkers; Care and treatment; Diagnosis; Disease control; Drug resistance; Drug therapy; Enzymes; Epidemics; Female; Health aspects; HIV; HIV infections; HIV Infections - blood; HIV Infections - epidemiology; HIV tests; Human immunodeficiency virus; Humans; Immunoassay; Immunoassay - instrumentation; Immunoassay - methods; Immunoglobulins; Infections; Infectious diseases; Longitudinal Studies; Male; Medicine and Health Sciences; Methods; Middle Aged; Oligonucleotides; Optical density; Prevention; Quebec - epidemiology; Research and Analysis Methods; Review boards; Substance abuse treatment; Surveillance; Canada; Montreal Quebec Canada; United States > US; Quebec Canada
• ISSN: 1932-6203; 1932-6203
• DOI: 10.1371/journal.pone.0156023

Accurate and practical biologic tools to estimate HIV incidence is crucial to better monitor the epidemic and evaluate the effectiveness of HIV prevention and treatment programs. We evaluated two avidity assays to measure recent HIV infection: the Sedia HIV-1 LAg-Avidity EIA (Sedia Biosciences, Portland) and the Centers for Disease Control and Prevention (CDC)-modified Bio-Rad-Avidity assay (Bio-Rad Laboratories, Mississauga, ON). Longitudinal specimens (n = 473) obtained from 123 treatment-naive seroconverted individuals enrolled in the Primary HIV-1 Infection (PHI) cohort of Quebec were used to determine the average time an individual is considered to be recently infected (mean duration of recent infection; MDRI), for the two avidity assays alone and in combination using a nonparametric survival method analysis. A total of 420 specimens from individuals with established HIV infection (90 individuals from the PHI cohort of Quebec and 330 individuals from the Laboratoire de santé publique du Quebec (LSPQ) serobank) were also tested to investigate false recency rate (FRR). The CDC-modified Bio-Rad-Avidity gave an estimated MDRI of 234 days (95% CI 220-249) at the avidity index cutoff of 30% while the Sedia-LAg-Avidity assay gave an estimated MDRI of 120 days (95% CI 109-132) at the normalized optical density (ODn) cutoff of 1.5. The FRR among individuals with established HIV infection was 10.2% (7.5%-13.5%) with the CDC-modified Bio-Rad-Avidity assay as compared to 6.0% (3.9%-8.7%) with the Sedia-LAg-Avidity assay. When optimizing a multiassay algorithm (MAA) that includes sequentially the CDC-modified Bio-Rad-Avidity assay then the Sedia-LAg-Avidity assay EIA (avidity index/ODn: 30%/1.7), the MDRI was 136 days (95% CI 123-148) and the FRR, 3.3% (95% CI 1.8-5.6). Multiassay algorithms that include the CDC-modified Bio-Rad-Avidity assay and the Sedia-LAg-Avidity assay performed better than each avidity assay alone. Such 2-assay algorithm that starts with the CDC-modified Bio-Rad-Avidity assay followed by the Sedia-LAg-Avidity assay allowed a better classification of HIV-1 infections.