Baseline cardiac troponin T positivity strongly predicted 30-day mortality (10% vs 0% in negative patients), and adding 8- and 16-hour measures significantly improved prognostic value (P=0.0036).
Cohort (n=734)
Does serial cardiac troponin T measurement improve prediction of 30-day and 1-year mortality in patients with acute coronary syndromes?
Serial measurements of cTnT at 8 and 16 hours provide additional prognostic value over baseline cTnT alone for predicting short-term mortality in acute coronary syndromes.
Tasa de eventos absoluta: 10% vs 0%
valor p: p=0.0113
BACKGROUND: The baseline cardiac troponin T (cTnT) level strongly predicts short-term mortality in acute coronary syndromes, but the added value of later measures to predict short- and long-term outcome and in the context of baseline clinical characteristics is unclear. METHODS AND RESULTS: Relations between baseline, peak, and 8- and 16-hour (late) cTnT results and outcomes were assessed in 734 patients in a GUSTO-IIa substudy. Proportional-hazards models assessed the prognostic information gained from late cTnT when added to a mortality model containing the baseline cTnT result and clinical factors. At baseline, 260 patients were cTnT-positive (>0.1 ng/mL), 323 became positive later, and 151 remained negative (</=0.1 ng/mL). Mortality at 30 days was 10% in the baseline-positive group, 5% in late-positive patients, and 0% in negative patients. After adjustment for baseline characteristics, any positive cTnT result predicted 30-day mortality (baseline, chi2=8.96, P=0.0113; 8-hour, chi2=6.51, P=0.0107; 16-hour, chi2=8.40, P=0.0038). Both the 8- and the 16-hour results added to the strength of the baseline result (baseline+8-hour, chi2=12.04, P=0.0072; baseline+16-hour, chi2=13.52, P=0.0036). Only age and ST-segment elevation were stronger predictors of 30-day mortality than baseline cTnT; results were similar for prediction of 1-year mortality. Most of the mortality difference between cTnT-positive and -negative patients occurred within the first 30 days. CONCLUSIONS: The cTnT level is a strong, independent predictor of short-term outcome in acute coronary syndromes. The addition of later samples to a baseline level is useful to evaluate the risk of serious cardiac events.
Newby et al. (Tue,) conducted a cohort in Acute Coronary Syndromes (n=734). Serial cardiac troponin T (cTnT) measures vs. Baseline cTnT alone or negative cTnT was evaluated on 30-day mortality (p=0.0113). Baseline cardiac troponin T positivity strongly predicted 30-day mortality (10% vs 0% in negative patients), and adding 8- and 16-hour measures significantly improved prognostic value (P=0.0036).
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