Infection staging and incidence surveillance applications of high dynamic range diagnostic immuno-assay platforms

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Date
2017-12
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Publisher
Wolters Kluwer
Abstract
Background: Custom HIV staging assays, including the Sedia HIV-1 Limiting Antigen (LAg) Avidity EIA and avidity modifications of the Ortho VITROS anti-HIV-1+2 and Abbott ARCHITECT HIV Ag/Ab Combo assays, are used to identify “recent” infections in clinical settings and for cross-sectional HIV incidence estimation. However, the high dynamic range of chemiluminescent platforms allows differentiating recent and long-standing infection on signal intensity, and this raises the prospect of using unmodified diagnostic assays for infection timing and surveillance applications. Methods: We tested a panel of 2500 well-characterized specimens with estimable duration of HIV infection with the 3 assays and the unmodified ARCHITECT. Regression models were used to estimate mean durations of recent infection (MDRIs), contextspecific false-recent rates (FRRs) and correlation between diagnostic signal intensity and LAg measurements. Hypothetical epidemiological scenarios were constructed to evaluate utility in surveillance applications. Results: Over a range of MDRIs (reflecting recency discrimination thresholds), a diluted ARCHITECT-based RITA produced lower FRRs than the VITROS platform (FRR z 0.5% and 1.5%, respectively at MDRI z 200 days), and the unmodified diagnostic ARCHITECT produces incidence estimates with comparable precision to LAg (relative SE z 17.5% and 15%, respectively at MDRIz 200 days). ARCHITECT S/CO measurements were highly correlated with LAg optical density measurements (r = 0.80), and values below 200 are strongly predictive of LAg recency and duration of infection less than 1 year. Conclusions: Low quantitative measurements from the unmodified ARCHITECT obviate the need for additional recency testing, and its use is feasible in clinical staging and incidence surveillance applications.
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CITATION: Grebe, E., Welte, A., Hall, J., Keating, S. M., Facente, S. N., Marson, K., Martin, J. N., Little, S. J., Price, M. A., Kallas, E. G., Busch, M. P., Pilcher, C. D., Murphy, G. on behalf of the Consortium for the Evaluation and Performance of HIV Incidence Assays (CEPHIA). Infection Staging and Incidence Surveillance Applications of High Dynamic Range Diagnostic Immuno-Assay Platforms. JAIDS Journal of Acquired Immune Deficiency Syndromes, 76(5):547-555. doi:10.1097/QAI.0000000000001537.
The original publication is available at https://journals.lww.com/jaids/pages/default.aspx
Keywords
Infection timing, Infection staging, Staging assays, Diagnostic assays
Citation
Grebe, E., Welte, A., Hall, J., Keating, S. M., Facente, S. N., Marson, K., Martin, J. N., Little, S. J., Price, M. A., Kallas, E. G., Busch, M. P., Pilcher, C. D., Murphy, G. on behalf of the Consortium for the Evaluation and Performance of HIV Incidence Assays (CEPHIA). Infection Staging and Incidence Surveillance Applications of High Dynamic Range Diagnostic Immuno-Assay Platforms. JAIDS Journal of Acquired Immune Deficiency Syndromes, 76(5):547-555. doi:10.1097/QAI.0000000000001537.
URI
http://hdl.handle.net/10019.1/101540
Collections
Research Articles ((SACEMA) South African Centre for Epidemiological Modelling and Analysis )