Determination of Mean Recency Period for Estimation of HIV Type 1 Incidence with the BED-Capture EIA in Persons Infected with Diverse Subtypes

Parekh, Bharat; Hanson, Debra L.; Hargrove, John W.; Branson, Bernard M.; Green, Timothy; Dobbs, Trudy; Constantine, Niel T.; Overbaugh, Julie; McDougal, J. Steven

doi:10.1089/aid.2010.0159

Cited by 82 publications

(113 citation statements)

References 30 publications

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“…First, total IgG levels are significantly higher in Africans than in individuals from Western countries due to exposure to multiple pathogens (39). This increased IgG level may interfere with the detection of p24 antigen due to nonspecific binding to the antigen.…”

Section: Discussionmentioning

confidence: 99%

Poor Performance of the Determine HIV-1/2 Ag/Ab Combo Fourth-Generation Rapid Test for Detection of Acute Infections in a National Household Survey in Swaziland

et al. 2014

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was lost to follow-up). Therefore, the Determine combo test had a sensitivity of 0% (95% confidence interval, 0 to 28) and positive predictive value of 0% for the detection of acute infections. The ability of the 4th-generation Determine combo to detect antigen was very poor in Swaziland. Thus, the Determine combo test does not add any value to the current testing algorithm; rather, it adds additional costs and complexity to HIV diagnosis. The detection of acute HIV infections may need to rely on other testing strategies.

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Section: Discussionmentioning

confidence: 99%

Poor Performance of the Determine HIV-1/2 Ag/Ab Combo Fourth-Generation Rapid Test for Detection of Acute Infections in a National Household Survey in Swaziland

et al. 2014

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“…17,19 The performance of serologic HIV incidence assays has been shown to vary by HIV subtype. [20][21][22][23] For example, among individuals infected for 2 or more years, being misclassified as assay positive is more likely in subtype D infection than subtype A infection. 18,24 In addition, among those with long-standing subtype D infection, women are significantly more likely to be misclassified as assay positive than men.…”

Section: Introductionmentioning

confidence: 99%

Impact of HIV Subtype on Performance of the Limiting Antigen-Avidity Enzyme Immunoassay, the Bio-Rad Avidity Assay, and the BED Capture Immunoassay in Rakai, Uganda

Longosz

Serwadda

Nalugoda

et al. 2014

AIDS Research and Human Retroviruses

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Previous studies demonstrated that individuals with subtype D HIV infection who had been infected for 2 or more years were frequently misclassified as assay positive using cross-sectional incidence assays. Samples from 510 subjects (212 subtype A, 298 subtype D) who were infected for 2.2 to 14.5 years (median 5.4 years) and were not virally suppressed were tested using an LAg-Avidity enzyme immunoassay (LAg-Avidity EIA), Bio-Rad Avidity assay, and BED capture enzyme immunoassay (BED-CEIA). The performance of these three assays was evaluated using various assay cutoff values [LAg-Avidity EIA: < 1.0 OD-n and < 2.0 OD-n; Bio-Rad Avidity assay: < 40% avidity index (AI) and < 80% AI; BED-CEIA: < 0.8 OD-n]. The mean LAg-Avidity EIA result was higher for subtype A than D (4.54 -0.95 vs. 3.86 -1.26, p < 0.001); the mean Bio-Rad Avidity assay result was higher for subtype A than D (88.9% -12.5% vs. 75.1 -30.5, p < 0.001); and the mean BED-CEIA result was similar for the two subtypes (2.2 -1.2 OD-n for subtype A, 2.2 -1.3 OD-n for subtype D, p < 0.9). The frequency of misclassification was higher for individuals with subtype D infection compared to those with subtype A infection, using either the LAg-Avidity EIA with a cutoff of < 2.0 OD-n or the Bio-Rad Avidity assay with cutoffs of < 40% or < 80% AI. No subtype-specific differences in assay performance were observed using the BED-CEIA. Sex and age were not significantly associated with misclassification by any assay. The LAg-Avidity EIA with a cutoff < 1.0 OD-n had the lowest frequency of misclassification in this Ugandan population.

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“…This allows recent and nonrecent infections to be distinguished by serology-based HIV-1 incidence assays in which the increase in the proportion of HIV-specific antibodies (2), the avidity of HIV-specific antibodies (3,4), or a combination of HIV-specific antibody level and avidity (5) is measured. Unfortunately, samples from individuals infected with HIV-1 non-B subtypes (6,7), from elite controllers (8), from individuals treated with antiretroviral drugs (8,9), and from individuals with advanced stages of disease (7,9) can be misclassified on the basis of serological criteria because of delayed or reduced production of HIV-specific antibodies. Nonserological HIV-1 incidence assays (10,11) and algorithms combining serological and nonserological biomarkers have therefore been developed (12,13).…”

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Assessment of Ambiguous Base Calls in HIV-1 pol Population Sequences as a Biomarker for Identification of Recent Infections in HIV-1 Incidence Studies

et al. 2014

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An increase in the proportion of ambiguous base calls in HIV-1 pol population sequences during the course of infection has been demonstrated in different study populations, and sequence ambiguity thresholds to classify infections as recent or nonrecent have been suggested. The aim of our study was to evaluate sequence ambiguities as a candidate biomarker for use in an HIV-1 incidence assay using samples from antiretroviral treatment-naive seroconverters with known durations of infection (German HIV-1 Seroconverter Study). We used 2,203 HIV-1 pol population sequences derived from 1,334 seroconverters to assess the sequence ambiguity method (SAM). We then compared the serological incidence BED capture enzyme immunoassay (BED-CEIA) with the SAM for a subset of 723 samples from 495 seroconverters and evaluated a multianalyte algorithm that includes BED-CEIA results, SAM results, viral loads, and CD4 cell counts for 453 samples from 325 seroconverters. We observed a significant increase in the proportion of sequence ambiguities with the duration of infection. A sequence ambiguity threshold of 0.5% best identified recent infections with 76.7% accuracy. The mean duration of recency was determined to be 208 (95% confidence interval, 196 to 221) days. In the subset analysis, BED-CEIA achieved a significantly higher accuracy than the SAM (84.6 versus 75.5%, P < 0.001) and results were concordant for 64.2% (464/723) of the samples. Also, the multianalyte algorithm did not show better accuracy than the BED-CEIA (83.4 versus 84.3%, P ‫؍‬ 0.786). In conclusion, the SAM and the multianalyte algorithm including SAM were inferior to the BED-CEIA, and the proportion of sequence ambiguities is therefore not a preferable biomarker for HIV-1 incidence testing.

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Determination of Mean Recency Period for Estimation of HIV Type 1 Incidence with the BED-Capture EIA in Persons Infected with Diverse Subtypes

Cited by 82 publications

References 30 publications

Poor Performance of the Determine HIV-1/2 Ag/Ab Combo Fourth-Generation Rapid Test for Detection of Acute Infections in a National Household Survey in Swaziland

Poor Performance of the Determine HIV-1/2 Ag/Ab Combo Fourth-Generation Rapid Test for Detection of Acute Infections in a National Household Survey in Swaziland

Impact of HIV Subtype on Performance of the Limiting Antigen-Avidity Enzyme Immunoassay, the Bio-Rad Avidity Assay, and the BED Capture Immunoassay in Rakai, Uganda

Assessment of Ambiguous Base Calls in HIV-1 pol Population Sequences as a Biomarker for Identification of Recent Infections in HIV-1 Incidence Studies

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