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Total observed error, total allowable error, and QC rules for canine serum and urine cortisol achievable with the Immulite 2000 Xpi cortisol immunoassay

Determining a simple quality control (QC) rule for daily performance monitoring depends on the desired total allowable error (TEa) for the measurand. When no consensus TEa exists, the classical approach of QC rule validation cannot be used. Using the results of previous canine serum and urine cortis...

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Autores principales: Korchia, Jeremie, Freeman, Kathleen P.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: SAGE Publications 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8921817/
https://www.ncbi.nlm.nih.gov/pubmed/35264042
http://dx.doi.org/10.1177/10406387221076129
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author Korchia, Jeremie
Freeman, Kathleen P.
author_facet Korchia, Jeremie
Freeman, Kathleen P.
author_sort Korchia, Jeremie
collection PubMed
description Determining a simple quality control (QC) rule for daily performance monitoring depends on the desired total allowable error (TEa) for the measurand. When no consensus TEa exists, the classical approach of QC rule validation cannot be used. Using the results of previous canine serum and urine cortisol validation studies on the Immulite 2000 Xpi, we applied a reverse engineering approach to QC rule determination, arbitrarily imposing sigma = 5, and determining the resulting TEa for the QC material (QCM; TEa(QCM)) and the resulting probability of error detection (P(ed)) for each QC rule. For the simple QC rule 1(2.5S) with P(ed) = 0.96 and probability of false rejection (P(fr)) = 0.03, the associated TEa(QCM) were 20% and 35% for serum and 28% and 24% for urine QCM1 and QCM2. If these levels of TEa(QCM) are acceptable for interpretation of patient sample results, then users can internally validate the 1(2.5S) QC rule, provided that their QCM CVs and biases are similar to ours. Otherwise, more stringent QC rules can be validated by using a lower sigma to lower the TEa(QCM). With spiked samples (relevant cortisol concentrations in the veterinary patient matrix) at 38.6 and 552 nmol/L of cortisol, TEa(QCM) at sigma = 5 were much higher (54% and 40% for serum; 90.3% and 42.8% for urine). Spiked samples generate TEa that is probably too high to be suitable for daily QC monitoring; however, it is crucial to verify spiked sample observed total error (TEo; 26% and 18% for serum, 60% and 30% for urine) < TEa(QCM), and to use spiked sample TEo for patient result interpretation. In the absence of consensus TEa for cortisol in dogs, we suggest the use of a 1(2.5S) rule, provided that users accept the associated level of TEa(QCM) also as clinical TEa for results interpretation.
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spelling pubmed-89218172022-05-25 Total observed error, total allowable error, and QC rules for canine serum and urine cortisol achievable with the Immulite 2000 Xpi cortisol immunoassay Korchia, Jeremie Freeman, Kathleen P. J Vet Diagn Invest Full Scientific Reports Determining a simple quality control (QC) rule for daily performance monitoring depends on the desired total allowable error (TEa) for the measurand. When no consensus TEa exists, the classical approach of QC rule validation cannot be used. Using the results of previous canine serum and urine cortisol validation studies on the Immulite 2000 Xpi, we applied a reverse engineering approach to QC rule determination, arbitrarily imposing sigma = 5, and determining the resulting TEa for the QC material (QCM; TEa(QCM)) and the resulting probability of error detection (P(ed)) for each QC rule. For the simple QC rule 1(2.5S) with P(ed) = 0.96 and probability of false rejection (P(fr)) = 0.03, the associated TEa(QCM) were 20% and 35% for serum and 28% and 24% for urine QCM1 and QCM2. If these levels of TEa(QCM) are acceptable for interpretation of patient sample results, then users can internally validate the 1(2.5S) QC rule, provided that their QCM CVs and biases are similar to ours. Otherwise, more stringent QC rules can be validated by using a lower sigma to lower the TEa(QCM). With spiked samples (relevant cortisol concentrations in the veterinary patient matrix) at 38.6 and 552 nmol/L of cortisol, TEa(QCM) at sigma = 5 were much higher (54% and 40% for serum; 90.3% and 42.8% for urine). Spiked samples generate TEa that is probably too high to be suitable for daily QC monitoring; however, it is crucial to verify spiked sample observed total error (TEo; 26% and 18% for serum, 60% and 30% for urine) < TEa(QCM), and to use spiked sample TEo for patient result interpretation. In the absence of consensus TEa for cortisol in dogs, we suggest the use of a 1(2.5S) rule, provided that users accept the associated level of TEa(QCM) also as clinical TEa for results interpretation. SAGE Publications 2022-03-09 2022-03 /pmc/articles/PMC8921817/ /pubmed/35264042 http://dx.doi.org/10.1177/10406387221076129 Text en © 2022 The Author(s)
spellingShingle Full Scientific Reports
Korchia, Jeremie
Freeman, Kathleen P.
Total observed error, total allowable error, and QC rules for canine serum and urine cortisol achievable with the Immulite 2000 Xpi cortisol immunoassay
title Total observed error, total allowable error, and QC rules for canine serum and urine cortisol achievable with the Immulite 2000 Xpi cortisol immunoassay
title_full Total observed error, total allowable error, and QC rules for canine serum and urine cortisol achievable with the Immulite 2000 Xpi cortisol immunoassay
title_fullStr Total observed error, total allowable error, and QC rules for canine serum and urine cortisol achievable with the Immulite 2000 Xpi cortisol immunoassay
title_full_unstemmed Total observed error, total allowable error, and QC rules for canine serum and urine cortisol achievable with the Immulite 2000 Xpi cortisol immunoassay
title_short Total observed error, total allowable error, and QC rules for canine serum and urine cortisol achievable with the Immulite 2000 Xpi cortisol immunoassay
title_sort total observed error, total allowable error, and qc rules for canine serum and urine cortisol achievable with the immulite 2000 xpi cortisol immunoassay
topic Full Scientific Reports
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8921817/
https://www.ncbi.nlm.nih.gov/pubmed/35264042
http://dx.doi.org/10.1177/10406387221076129
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