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首页> 外文期刊>Thrombosis Research: An International Journal on Vascular Obstruction, Hemorrhage and Hemostasis >The flow cytometer model markedly affects measurement of ex vivo whole blood platelet-bound P-selectin expression in patients with chest pain: are we comparing apples with oranges.
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The flow cytometer model markedly affects measurement of ex vivo whole blood platelet-bound P-selectin expression in patients with chest pain: are we comparing apples with oranges.

机译:流式细胞仪模型明显影响胸痛患者离体全血血小板结合的P-选择素表达的测量:我们是否将苹果与橘子进行比较。

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摘要

Surface expression of P-selectin is known to be a marker of platelet activation in patients with acute coronary syndromes. However, direct comparisons of flow cytometer data may be obscured by differences in methodology, artifactual platelet activation during washing procedures, choice of antibodies, absence of control measurements, and possible observer bias due to unblinded data collection. We sought to test the hypothesis that the model of flow cytometer represents another variable affecting P-selectin measurements. Platelet P-selectin in whole blood was measured by FACScan (Becton Dickinson, Inc., San Diego, CA, USA) or EPICS XL (Coulter Corporation, Hialeah, FL, USA) flow cytometry in 338 patients presenting with chest pain to the emergency departments of three community hospitals as part of a multicenter diagnostic trial. Platelet expression of P-selectin (% of cell positivity) was consistently higher for each discharge diagnosis when measured with FACScan flow cytometer (13.2+/-4.1 for myocardial infarction, 10.0+/-3.6 for unstable angina, 9.9+/-3.5 for heart failure, 4.7+/-0.1 for gastrointestinal illness, and 6.3+/-0.7 for patients with noncardiac chest pain) when compared with results obtained from the EPICS XL instrument (2.4+/-0.2, 2.5+/-0.2, 2.5+/-0.1, 1.8+/-0.1, and 2.3+/-0.1 respectively, p=0.0001 for all groups). This study reveals marked discrepancies in the level of platelet P-selectin measurement based exclusively on the model of flow cytometer used. If P-selectin is to become a diagnostic tool for differentiating an etiology of chest pain, standardized measurements must be defined for each model of flow cytometer.
机译:已知P-选择蛋白的表面表达是急性冠脉综合征患者血小板活化的标志。但是,流式细胞仪数据的直接比较可能会因方法上的差异,清洗程序中的人工血小板活化,抗体的选择,对照测量的缺乏以及由于无盲数据收集而可能引起的观察者偏倚而被遮盖。我们试图验证流式细胞仪模型代表另一个影响P-选择素测量的变量的假设。通过FACScan(Becton Dickinson,Inc.,San Diego,CA,USA)或EPICS XL(Coulter Corporation,Hialeah,FL,USA)流式细胞术对338例急诊出现胸痛的患者进行全血血小板P选择素测定作为多中心诊断试验的一部分,三个社区医院的医院部门。用FACScan流式细胞仪测量时,每次出院诊断时P-选择素的血小板表达(细胞阳性率)始终较高(心肌梗塞为13.2 +/- 4.1,不稳定型心绞痛为10.0 +/- 3.6,9.9±3.5)。与使用EPICS XL仪器获得的结果相比(2.4 +/- 0.2、2.5 +/- 0.2、2.5+ /-0.1、1.8+/-0.1和2.3 +/- 0.1,对于所有组,p = 0.0001)。这项研究仅基于所使用的流式细胞仪模型揭示了血小板P-选择素测量水平的显着差异。如果P选择素要成为区分胸痛病因的诊断工具,则必须为每种流式细胞仪模型定义标准化的测量方法。

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