新型第三代高敏肌钙蛋白 I 检测方法用于急性非 ST 段抬高型心肌梗死的 90 分钟即时诊断性能和 30 天预后评估。
Short-term (90 min) diagnostic performance for acute non-ST segment elevation myocardial infarction and 30-day prognostic evaluation of a novel third-generation high sensitivity troponin I assay.
机构信息
Division of Emergency Medicine, Stanford University School of Medicine, Stanford, CA 94305-2200, United States.
出版信息
Clin Biochem. 2012 Nov;45(16-17):1295-301. doi: 10.1016/j.clinbiochem.2012.06.005. Epub 2012 Jun 15.
OBJECTIVES
We evaluated a third-generation high sensitivity "guidelines acceptable" troponin I assay (hs-cTnI) against a contemporary "clinically usable" troponin assay (cTnI).
DESIGN AND METHODS
Remnant samples of undifferentiated emergency department (ED) patients with suspected acute coronary syndrome were enrolled. Baseline and 90-minute samples were analyzed for cTnI and hs-cTnI. Sensitivity, specificity, positive and negative predictive values for AMI and 30-day adverse cardiac events (ACE) were compared.
RESULTS
Of 486 ED patients, there were 465 patients who had blood remaining at the presentation for the hs-cTnI assays, with 12 AMIs. At presentation, the clinical sensitivity and specificity for AMI was 75% and 97% for cTnI and 83.3 and 82.1% for hs-cTnI. There were 407 patients who had paired baseline and 90-minute blood samples for cTnI and hs-cTnI including 9 of the 12 AMI patients. The sensitivity and specificity was 77.7% and 96.5% for cTnI and 100% and 81.9% for hs-cTnI at 90 min. A Δ change of 30% increase from baseline to 90 min improved the specificity to 94.5% (95% CI 92%-96%) without lowering the sensitivity. When AMI was defined as a Δ30% change of hs-cTnI at t=0 and 90 min and one hs-cTnI result >99th percentile cutoff, more than 3 times as many patients met the diagnostic criteria for AMI compared to results from the normal sensitive troponin assay; 28 (6.9%) for hs-cTnI vs. 9 (2.2%) with cTnI. There were 37 in-hospital or 30-day events, producing an OR of 3.03, 95% CI: 0.86-9.59 for cTnI, and 2.54, 95% CI: 1.27-5.10 for hs-cTnI, which detected 11 more cases.
CONCLUSIONS
The hs-cTnI assay achieved a 90-minute rule out for AMI and detected more 3 times as many AMI cases. The specificity increased with the Δ30% criteria. The hs-cTnI assay also detected more cases of patient at risk for adverse cardiac events at 30 days.
目的
我们评估了第三代高敏“指南可接受”肌钙蛋白 I 测定法(hs-cTnI)与当代“临床可用”肌钙蛋白测定法(cTnI)的比较。
设计和方法
招募疑似急性冠状动脉综合征的未分化急诊患者的残余样本。对 cTnI 和 hs-cTnI 进行基线和 90 分钟样本分析。比较 AMI 和 30 天不良心脏事件(ACE)的敏感性、特异性、阳性和阴性预测值。
结果
在 486 名 ED 患者中,有 465 名患者在就诊时留有 hs-cTnI 检测的血液,其中有 12 例 AMI。在就诊时,cTnI 对 AMI 的临床敏感性和特异性分别为 75%和 97%,hs-cTnI 为 83.3%和 82.1%。有 407 名患者同时进行了基线和 90 分钟的 cTnI 和 hs-cTnI 配对血样检测,其中包括 12 例 AMI 患者中的 9 例。90 分钟时,cTnI 的敏感性和特异性分别为 77.7%和 96.5%,hs-cTnI 的敏感性和特异性分别为 100%和 81.9%。从基线到 90 分钟时,hs-cTnI 的变化增加 30%可将特异性提高到 94.5%(95%CI 92%-96%),而不降低敏感性。当 AMI 定义为 hs-cTnI 在 t=0 和 90 分钟时增加 30%和一个 hs-cTnI 结果超过 99 百分位截止值时,与正常敏感肌钙蛋白检测相比,符合 AMI 诊断标准的患者数量增加了 3 倍以上;hs-cTnI 为 28 例(6.9%),cTnI 为 9 例(2.2%)。住院或 30 天内有 37 例事件,OR 为 3.03,95%CI:0.86-9.59 为 cTnI,2.54,95%CI:1.27-5.10 为 hs-cTnI,检测到 11 例更多病例。
结论
hs-cTnI 检测法可在 90 分钟内排除 AMI,并检测到 3 倍以上的 AMI 病例。特异性随Δ30%标准而增加。hs-cTnI 检测法还检测到 30 天内更多的不良心脏事件风险患者。
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