Utility of Antinuclear Antibody Screening by Various Methods in a Clinical Laboratory Patient Cohort

Duan, Xiaoli; Peters, Barbara J.; Ettore, Michael W.; Ashworth, Judy; Brunelle, Lynn A; Crowson, Cynthia S.; Moder, Kevin G.; Snyder, Melissa R.

doi:10.1373/jalm.2016.020172

Cited by 14 publications

(18 citation statements)

References 26 publications

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“…However, this scenario is rarely the case for the hemolysis/icterus/ lipemia (HIL) 1 index analysis because of its integrated, automated use on the chemistry/immunochemistry platforms. The HIL index analyses seldom has predefined demands to quality performance, meaning that…”

Section: Hemolysis-icteruslipemia Index Analysis: a National Survey Omentioning

confidence: 99%

In Response to: Utility of Antinuclear Antibody Screening by Various Methods in a Clinical Laboratory Patient Cohort—Differences in Sensitivity, Specificity, and Limitations

Hall¹,

Hoy²,

DiMaio³

2017

The Journal of Applied Laboratory Medicine

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Section: Hemolysis-icteruslipemia Index Analysis: a National Survey Omentioning

confidence: 99%

In Response to: Utility of Antinuclear Antibody Screening by Various Methods in a Clinical Laboratory Patient Cohort—Differences in Sensitivity, Specificity, and Limitations

Hall¹,

Hoy²,

DiMaio³

2017

The Journal of Applied Laboratory Medicine

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“…The authors would like to thank Dr. Baird for his constructive comments regarding the calculation of sensitivity and specificity of antinuclear antibody (ANA) 1 testing in our recent publication (1). The goal of this study was to compare the diagnostic utility of various ANA methods in a representative testing population.…”

Section: In Reply To Geoffrey Baird On: Utility Of Antinuclear Antibomentioning

confidence: 99%

In Response to: Utility of Antinuclear Antibody Screening by Various Methods in a Clinical Laboratory Patient Cohort

Baird

2016

The Journal of Applied Laboratory Medicine

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“…This trend is reflected in recent literature and the updated 2015 American College of Rheumatology (ACR) position statement on ANA testing (4,8). Our institution implemented EIA-based ANA screens in July of 2015 as a way to focus manual IFA testing on specimens more likely to be positive.…”

mentioning

confidence: 99%

“…IFA using HEp-2 substrate is considered the gold standard method for clinical ANA testing (2)(3)(4); it is historically a manual technique with some automation recently available in the US market. MIA and EIA are generally more automatable than IFA and have variable sensitivity for CTD depending on how they are configured (2,3,(5)(6)(7)(8).…”

mentioning

confidence: 99%

Quality Monitoring Approach for Optimizing Antinuclear Antibody Screening Cutoffs and Testing Work Flow

Tacker

Perrotta

2017

The Journal of Applied Laboratory Medicine

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Background An antinuclear antibody (ANA) testing strategy involving enzyme immunoassay (EIA) screening that reflexed to immunofluorescence assay (IFA) was implemented, monitored, and optimized for clinical utility. Methods The clinical utility, test performance, and workload implications of various ANA testing strategies were compared during the following study phases: (a) Preimplementation (n = 469) when IFA was used for all ANA screening, (b) Verification (n = 58) when EIA performance was confirmed, (c) Implementation (n = 433) when a reflexive strategy (EIA screen/IFA confirmation) was implemented, and (d) Postimplementation (n = 528) after the reflexive strategy was optimized. Sequential samples were captured in the Preimplementation, Implementation, and Postimplementation phases for clinical performance evaluation. Results Clinical performance of the EIA screen, per ROC analysis yielded area under the curve (AUC) of 0.846 in the Implementation phase and increased to 0.934 Postimplementation (P < 0.01); AUC for IFA similarly increased, from 0.678 to 0.808 (P = 0.05). The reflexive testing strategy increased screening sensitivity from 61% Preimplementation (IFA) to 98% (EIA) at Implementation and was maintained after optimization (98%, Postimplementation). Optimization decreased the false-positive rates for both EIA (from 40% to 18%) and IFA (18% to 8%) and was associated with reductions in daily full-time equivalent (by 33%) and IFA slide use (by 50%). Conclusions Continuous quality monitoring approaches that incorporate sequential data sets can be used to evaluate, deploy, and optimize sensitive EIA-based ANA screening methods that can reduce manual IFA work without sacrificing clinically utility.

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Utility of Antinuclear Antibody Screening by Various Methods in a Clinical Laboratory Patient Cohort

Cited by 14 publications

References 26 publications

In Response to: Utility of Antinuclear Antibody Screening by Various Methods in a Clinical Laboratory Patient Cohort—Differences in Sensitivity, Specificity, and Limitations

In Response to: Utility of Antinuclear Antibody Screening by Various Methods in a Clinical Laboratory Patient Cohort—Differences in Sensitivity, Specificity, and Limitations

In Response to: Utility of Antinuclear Antibody Screening by Various Methods in a Clinical Laboratory Patient Cohort

Quality Monitoring Approach for Optimizing Antinuclear Antibody Screening Cutoffs and Testing Work Flow

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