Simulation models predicted that low hs-cTnI thresholds (2-5 ng/L) are prone to misclassification rates of 5%-10%, whereas thresholds near the 99th percentile (26.2 ng/L) have rates of 0.4%-0.6%.
How do assay bias and imprecision affect the misclassification rate of myocardial infarction at various high-sensitivity cardiac troponin I thresholds?
Simulation models suggest that low hs-cTnI thresholds (2-5 ng/L) are prone to higher misclassification rates (5-10%) due to assay bias compared to higher thresholds near the 99th percentile (<1%).
BACKGROUND: Clinical outcome studies for cardiac troponins (cTn) are expensive and difficult to design owing to variation in patients, in the assays, and in the incidence of different types of myocardial infarction (MI). To overcome these difficulties, simulation models were used to estimate the rate of misclassification error for MI and risk prediction resulting from assay bias and imprecision. METHODS: Finite mixture analysis of Abbott high-sensitivity cTnI (hs-cTnI) results at time 0 h in patients presenting early with acute coronary syndrome (ACS) symptoms to the emergency department (ED) n = 145, Reducing the Time Interval for Identifying New Guideline (RING) study allowed derivation of a simulation data set (n = 10000). hs-cTnI concentrations were modified by addition of bias or imprecision error. The percentage of all 10000 modified hs-cTnI results that were misclassified for MI at thresholds of 2, 5, 26.2, and 52 ng/L was determined by Monte Carlo simulation. Analyses were replicated with an all-comer emergency department (ED) population (n = 1137) ROMI (Optimum Troponin Cutoffs for ACS in the ED) study. RESULTS: In the RING study, simulation at 26.2-ng/L (99th percentile) and 52-ng/L thresholds were affected by both bias ±2 ng/L and imprecision (10%-20%) and had misclassification rates of 0.4% to 0.6%. Simulations at the 2-ng/L and 5-ng/L thresholds were only affected by bias. Misclassification rates at bias of ±1 ng/L were 10% for the 2-ng/L threshold, and 5% for the 5-ng/L threshold. CONCLUSIONS: Simulation models predicted that hs-cTnI results are seldom misclassified (<1% of patients) when interpretative thresholds are near or exceed the overall 99th percentile. However, simulation models also predicted that low hs-cTnI results, as recommended in guidelines, are prone to misclassification of 5%-10% of patients.
Lyon et al. (Wed,) conducted a other in Acute coronary syndrome (ACS) symptoms (n=10,000). Simulation models of hs-cTnI assay bias and imprecision was evaluated on Percentage of modified hs-cTnI results misclassified for MI at thresholds of 2, 5, 26.2, and 52 ng/L. Simulation models predicted that low hs-cTnI thresholds (2-5 ng/L) are prone to misclassification rates of 5%-10%, whereas thresholds near the 99th percentile (26.2 ng/L) have rates of 0.4%-0.6%.
Synapse has enriched 5 closely related papers on similar clinical questions. Consider them for comparative context: