Performance comparison of the Maxim and Sedia Limiting Antigen Avidity assays for HIV incidence surveillance

BACKGROUND: Two manufacturers, Maxim Biomedical and Sedia Biosciences Corporation, supply CDC-approved versions of the HIV-1 Limiting Antigen Avidity EIA (LAg) for detecting ‘recent’ HIV infection in cross-sectional incidence estimation. This study assesses and compares the performance of the two as...

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Autores principales: Sempa, Joseph B., Welte, Alex, Busch, Michael P., Hall, Jake, Hampton, Dylan, Facente, Shelley N., Keating, Sheila M., Marson, Kara, Parkin, Neil, Pilcher, Christopher D., Murphy, Gary, Grebe, Eduard
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2019
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6660077/
https://www.ncbi.nlm.nih.gov/pubmed/31348809
http://dx.doi.org/10.1371/journal.pone.0220345
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author Sempa, Joseph B.
Welte, Alex
Busch, Michael P.
Hall, Jake
Hampton, Dylan
Facente, Shelley N.
Keating, Sheila M.
Marson, Kara
Parkin, Neil
Pilcher, Christopher D.
Murphy, Gary
Grebe, Eduard
author_facet Sempa, Joseph B.
Welte, Alex
Busch, Michael P.
Hall, Jake
Hampton, Dylan
Facente, Shelley N.
Keating, Sheila M.
Marson, Kara
Parkin, Neil
Pilcher, Christopher D.
Murphy, Gary
Grebe, Eduard
author_sort Sempa, Joseph B.
collection PubMed
description BACKGROUND: Two manufacturers, Maxim Biomedical and Sedia Biosciences Corporation, supply CDC-approved versions of the HIV-1 Limiting Antigen Avidity EIA (LAg) for detecting ‘recent’ HIV infection in cross-sectional incidence estimation. This study assesses and compares the performance of the two assays for incidence surveillance. METHODS: We ran both assays on a panel of 2,500 well-characterized HIV-1-infected specimens. We analysed concordance of assay results, assessed reproducibility using repeat testing and estimated mean durations of recent infection (MDRIs) and false-recent rates (FRRs) for a range of normalized optical density (ODn) thresholds, alone and in combination with viral load thresholds. We defined three hypothetical surveillance scenarios, similar to the Kenyan and South African epidemics, and a concentrated epidemic. These scenarios allowed us to evaluate the precision of incidence estimates obtained by means of various recent infection testing algorithms (RITAs) based on each of the two assays. RESULTS: The Maxim assay produced lower ODn values than the Sedia assay on average, largely as a result of higher calibrator readings (mean OD of 0.749 vs. 0.643), with correlation of normalized readings lower (R(2) = 0.908 vs. R(2) = 0.938). Reproducibility on blinded control specimens was slightly better for Maxim. The MDRI of a Maxim-based algorithm at the ‘standard’ threshold (ODn ≤1.5 & VL >1,000) was 201 days (95% CI: 180,223) and for Sedia 171 (152,191). The difference Differences in MDRI were estimated at 32.7 (22.9,42.8) and 30.9 days (21.7,40.7) for the two algorithms, respectively. Commensurately, the Maxim algorithm had a higher FRR in treatment-naive subjects (1.7% vs. 1.1%). The two assays produced similar precision of incidence estimates in the three surveillance scenarios. CONCLUSIONS: Differences between the assays can be primarily attributed to the calibrators supplied by the manufacturers. Performance for surveillance was extremely similar, although different thresholds were optimal (i.e. produced the lowest variance of incidence estimates) and at any given ODn threshold, different estimates of MDRI and FRR were obtained. The two assays cannot be treated as interchangeable: assay and algorithm-specific performance characteristic estimates must be used for survey planning and incidence estimation.
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spelling pubmed-66600772019-08-07 Performance comparison of the Maxim and Sedia Limiting Antigen Avidity assays for HIV incidence surveillance Sempa, Joseph B. Welte, Alex Busch, Michael P. Hall, Jake Hampton, Dylan Facente, Shelley N. Keating, Sheila M. Marson, Kara Parkin, Neil Pilcher, Christopher D. Murphy, Gary Grebe, Eduard PLoS One Research Article BACKGROUND: Two manufacturers, Maxim Biomedical and Sedia Biosciences Corporation, supply CDC-approved versions of the HIV-1 Limiting Antigen Avidity EIA (LAg) for detecting ‘recent’ HIV infection in cross-sectional incidence estimation. This study assesses and compares the performance of the two assays for incidence surveillance. METHODS: We ran both assays on a panel of 2,500 well-characterized HIV-1-infected specimens. We analysed concordance of assay results, assessed reproducibility using repeat testing and estimated mean durations of recent infection (MDRIs) and false-recent rates (FRRs) for a range of normalized optical density (ODn) thresholds, alone and in combination with viral load thresholds. We defined three hypothetical surveillance scenarios, similar to the Kenyan and South African epidemics, and a concentrated epidemic. These scenarios allowed us to evaluate the precision of incidence estimates obtained by means of various recent infection testing algorithms (RITAs) based on each of the two assays. RESULTS: The Maxim assay produced lower ODn values than the Sedia assay on average, largely as a result of higher calibrator readings (mean OD of 0.749 vs. 0.643), with correlation of normalized readings lower (R(2) = 0.908 vs. R(2) = 0.938). Reproducibility on blinded control specimens was slightly better for Maxim. The MDRI of a Maxim-based algorithm at the ‘standard’ threshold (ODn ≤1.5 & VL >1,000) was 201 days (95% CI: 180,223) and for Sedia 171 (152,191). The difference Differences in MDRI were estimated at 32.7 (22.9,42.8) and 30.9 days (21.7,40.7) for the two algorithms, respectively. Commensurately, the Maxim algorithm had a higher FRR in treatment-naive subjects (1.7% vs. 1.1%). The two assays produced similar precision of incidence estimates in the three surveillance scenarios. CONCLUSIONS: Differences between the assays can be primarily attributed to the calibrators supplied by the manufacturers. Performance for surveillance was extremely similar, although different thresholds were optimal (i.e. produced the lowest variance of incidence estimates) and at any given ODn threshold, different estimates of MDRI and FRR were obtained. The two assays cannot be treated as interchangeable: assay and algorithm-specific performance characteristic estimates must be used for survey planning and incidence estimation. Public Library of Science 2019-07-26 /pmc/articles/PMC6660077/ /pubmed/31348809 http://dx.doi.org/10.1371/journal.pone.0220345 Text en © 2019 Sempa et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Sempa, Joseph B.
Welte, Alex
Busch, Michael P.
Hall, Jake
Hampton, Dylan
Facente, Shelley N.
Keating, Sheila M.
Marson, Kara
Parkin, Neil
Pilcher, Christopher D.
Murphy, Gary
Grebe, Eduard
Performance comparison of the Maxim and Sedia Limiting Antigen Avidity assays for HIV incidence surveillance
title Performance comparison of the Maxim and Sedia Limiting Antigen Avidity assays for HIV incidence surveillance
title_full Performance comparison of the Maxim and Sedia Limiting Antigen Avidity assays for HIV incidence surveillance
title_fullStr Performance comparison of the Maxim and Sedia Limiting Antigen Avidity assays for HIV incidence surveillance
title_full_unstemmed Performance comparison of the Maxim and Sedia Limiting Antigen Avidity assays for HIV incidence surveillance
title_short Performance comparison of the Maxim and Sedia Limiting Antigen Avidity assays for HIV incidence surveillance
title_sort performance comparison of the maxim and sedia limiting antigen avidity assays for hiv incidence surveillance
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6660077/
https://www.ncbi.nlm.nih.gov/pubmed/31348809
http://dx.doi.org/10.1371/journal.pone.0220345
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