Short-and Long-Term Biological Variation in Cardiac Troponin I Measured with a High-Sensitivity Assay : Implications for Clinical Practice

The improved detection limit and precision in new-generation commercial assays for cardiac troponin I (cTnI) have lowered the 99th-percentile cutoff value, yielding higher frequencies of positive test results. Because serial testing is important in interpreting low concentrations, we evaluated the b...

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Veröffentlicht in:Clinical chemistry (Baltimore, Md.) Md.), 2009, Vol.55 (1), p.52-58
Hauptverfasser: WU, Alan H. B, ANH LU, Quynh, TODD, John, MOECKS, Joachim, WIANS, Frank
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creator WU, Alan H. B
ANH LU, Quynh
TODD, John
MOECKS, Joachim
WIANS, Frank
description The improved detection limit and precision in new-generation commercial assays for cardiac troponin I (cTnI) have lowered the 99th-percentile cutoff value, yielding higher frequencies of positive test results. Because serial testing is important in interpreting low concentrations, we evaluated the biological variation of cTnI in both the short (hours) and long (weeks) terms and determined reference change values (RCVs) and the index of individuality (II) for cTnI. To assess short- and long-term variation, we collected blood from 12 healthy volunteers hourly for 4 h and from 17 healthy individuals once every other week for 8 weeks, measured cTnI with a high-sensitivity assay (detection limit, 0.2 ng/L), and computed analytical, intraindividual, interindividual, and total CVs (CV(A), CV(I), CV(G), and CV(T), respectively; CV(T) = CV(A) + CV(I) + CV(G)) as well as the II. Because of the slight right-skewness of the data, RCVs were calculated with a lognormal approach. Within-day CV(A), CV(I), and CV(G) values were 8.3%, 9.7%, and 57%, respectively; the corresponding between-day values were 15%, 14%, and 63%. Within- and between-day IIs were 0.21 and 0.39, respectively. Lognormal within-day RCVs were 46% and -32%, respectively; the corresponding between-day values were 81% and -45%. The low II indicates that population-based reference intervals are less useful for interpreting cTnI values than following serial changes in values in individual patients. This criterion is particularly important for interpreting results from patients who show cTnI increases at low concentrations measured with very high-sensitivity assays, from patients presenting with chest pain (short term), and for evaluating drugs for cardiotoxicity (long term).
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Because serial testing is important in interpreting low concentrations, we evaluated the biological variation of cTnI in both the short (hours) and long (weeks) terms and determined reference change values (RCVs) and the index of individuality (II) for cTnI. To assess short- and long-term variation, we collected blood from 12 healthy volunteers hourly for 4 h and from 17 healthy individuals once every other week for 8 weeks, measured cTnI with a high-sensitivity assay (detection limit, 0.2 ng/L), and computed analytical, intraindividual, interindividual, and total CVs (CV(A), CV(I), CV(G), and CV(T), respectively; CV(T) = CV(A) + CV(I) + CV(G)) as well as the II. Because of the slight right-skewness of the data, RCVs were calculated with a lognormal approach. Within-day CV(A), CV(I), and CV(G) values were 8.3%, 9.7%, and 57%, respectively; the corresponding between-day values were 15%, 14%, and 63%. Within- and between-day IIs were 0.21 and 0.39, respectively. Lognormal within-day RCVs were 46% and -32%, respectively; the corresponding between-day values were 81% and -45%. The low II indicates that population-based reference intervals are less useful for interpreting cTnI values than following serial changes in values in individual patients. This criterion is particularly important for interpreting results from patients who show cTnI increases at low concentrations measured with very high-sensitivity assays, from patients presenting with chest pain (short term), and for evaluating drugs for cardiotoxicity (long term).</abstract><cop>Washington, DC</cop><pub>American Association for Clinical Chemistry</pub><pmid>18988755</pmid><doi>10.1373/clinchem.2008.107391</doi><tpages>7</tpages><oa>free_for_read</oa></addata></record>
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subjects Adult
Analytical, structural and metabolic biochemistry
Biological and medical sciences
Biological variation
Biomarkers - blood
Cardiology
Cardiovascular disease
Clinical Medicine - standards
Cohort Studies
Emergency medical care
Female
Fundamental and applied biological sciences. Psychology
Heart attacks
Humans
Immunoassay
Investigative techniques, diagnostic techniques (general aspects)
Male
Medical sciences
Middle Aged
Reference Values
Reproducibility of Results
Sensitivity and Specificity
Time Factors
Troponin I - blood
title Short-and Long-Term Biological Variation in Cardiac Troponin I Measured with a High-Sensitivity Assay : Implications for Clinical Practice
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