Wilson Sean R, Sabatine Marc S, Braunwald Eugene, Sloan Sarah, Murphy Sabina A, Morrow David A
TIMI Study Group, Brigham and Women's Hospital and Department of Medicine, Boston, MA 02115, USA.
Am Heart J. 2009 Sep;158(3):386-91. doi: 10.1016/j.ahj.2009.06.011. Epub 2009 Jul 15.
At least 30% of patients with non-ST-elevation acute coronary syndrome present without evidence of myonecrosis using current generation troponin assays. A new generation of research assays for troponin that offer a >10-fold increase in analytical sensitivity has emerged.
To perform a pilot study to evaluate the clinical sensitivity of a new ultra-sensitive nanoparticle assay for cardiac troponin I (nano-cTnI), we identified 50 patients with unstable angina (serial negative cTnI) and 50 patients with non-ST-elevation myocardial infarction with an initially negative current generation cTnI result. We measured cTnI using an assay (Nanosphere, Northbrook, IL) that can detect pg/mL concentrations of cTnI (detection-limit 0.0002 microg/L).
Measured at 0, 2, and 8 hours with the nano-cTnI assay 44%, 62%, and 82% of patients with unstable angina defined by the current-generation assay had an elevated nano-cTnI result (> or =0.003 microg/L, 99 th percentile decision-limit, coefficient of variation <10%). In patients with definite myocardial injury (current-generation cTnI > or =0.1 microg/L) but an initially negative cTnI, 72% and 98% had a nano-cTnI > or =0.003 microg/L at 0 and 2 hours. No patient had a positive current-generation cTnI without an elevated nano-cTnI level.
In this pilot study using a nanoparticle assay for cTnI, myocardial injury was detectable in a substantial proportion of patients presently classified as having unstable angina, suggesting that ischemia with rest pain without injury is rare. The emergence of a new generation of troponin assays has the potential to lead to new clinical applications based on enhanced analytical performance at very low concentrations of troponin.
使用当前一代肌钙蛋白检测方法,至少30%的非ST段抬高型急性冠状动脉综合征患者并无心肌坏死证据。新一代肌钙蛋白研究检测方法已出现,其分析灵敏度提高了10倍以上。
为开展一项初步研究以评估一种新型超灵敏纳米颗粒心肌肌钙蛋白I检测方法(纳米cTnI)的临床灵敏度,我们确定了50例不稳定型心绞痛患者(连续cTnI阴性)和50例非ST段抬高型心肌梗死患者,其当前一代cTnI结果最初为阴性。我们使用一种能够检测pg/mL浓度cTnI(检测限0.0002μg/L)的检测方法(Nanosphere,美国伊利诺伊州诺斯布鲁克)来测量cTnI。
使用纳米cTnI检测方法在0小时、2小时和8小时测量时,当前一代检测方法定义的不稳定型心绞痛患者中,分别有44%、62%和82%的患者纳米cTnI结果升高(≥0.003μg/L,第99百分位数判定限,变异系数<10%)。在明确心肌损伤(当前一代cTnI≥0.1μg/L)但最初cTnI为阴性的患者中,0小时和2小时时分别有72%和98%的患者纳米cTnI≥0.003μg/L。没有患者当前一代cTnI呈阳性而纳米cTnI水平未升高。
在这项使用纳米颗粒检测cTnI的初步研究中,目前被归类为不稳定型心绞痛的相当一部分患者可检测到心肌损伤,这表明无损伤的静息性疼痛性缺血很少见。新一代肌钙蛋白检测方法的出现有可能基于在极低浓度肌钙蛋白时增强的分析性能而带来新的临床应用。
