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Assessment and diagnostic relevance of novel serum biomarkers for early decision of ST-elevation myocardial infarction

机译:新型血清生物标志物对ST抬高型心肌梗死早期判定的评估和诊断意义

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摘要

Blood transcriptome reflects the status of diseases, and characteristic molecular signature provides a novel window on gene expression preceding acute coronary events. We aim to determine blood transcriptome-based molecular signature of acute coronary syndrome (ACS), and to identify novel serum biomarkers for early stage ST-segment-elevation myocardial infarction (STEMI). We obtained peripheral blood from the patients with ACS who visited emergency department within 4 hours after the onset of chest pain: STEMI (n = 10), Non-ST-segment-elevation MI (NSTEMI, n = 10) and unstable angina (UA, n = 11). Blood transcriptome scans revealed that a characteristic gene expression change exists in STEMI, resulting in 531 outlier genes as STEMI molecular signature (Welch's t test, P < 0.05). Another analysis with a set of blood samples of patients with STEMI (n = 7) before and 7 days after the primary percutaneous coronary intervention (n = 7) and normal control (n = 10) evidenced that STEMI molecular signature directly reflects the onset of STEMI pathogenesis. From the two sets of transcriptome-based STEMI signatures, we identified 10 genes encoding transmembrane or secretory proteins that are highly expressed in STEMI. We validated blood protein expression levels of these 10 putative biomarkers in 40 STEMI and 32 healthy subjects by ELISA. Data suggested that PGLYRP1, IRAK3 and VNN3 are more specific and sensitive diagnostic biomarkers for STEMI than traditional CK-MB or troponin.Blood transcriptome scans of ACS evidenced early stage molecular markers for STEMI. Here, we report novel biomarkers to diagnose STEMI at emergency department in hospitals by a simple ELISA method.
机译:血液转录组反映疾病的状况,特征性分子标记为急性冠状动脉事件发生前的基因表达提供了一个新的窗口。我们的目标是确定基于血液转录组的急性冠状动脉综合征(ACS)的分子标记,并确定早期ST段抬高型心肌梗死(STEMI)的新型血清生物标志物。我们从ACS患者中获取了外周血,这些患者在胸痛发作后4小时内就诊了急诊科:STEMI(n = 10),非ST段抬高型MI(NSTEMI,n = 10)和不稳定型心绞痛(UA) ,n = 11)。血液转录组扫描显示,STEMI中存在特征基因表达变化,从而导致531个异常基因成为STEMI分子标记(Welch's t检验,P <0.05)。在原发性经皮冠状动脉介入治疗(n = 7)和正常对照(n = 10)之前和之后的7天,对一组STEMI患者(n = 7)的血液样本进行的另一项分析表明,STEMI分子标记直接反映了STEMI的发作。 STEMI的发病机制。从两组基于转录组的STEMI签名中,我们确定了10个编码跨膜或分泌蛋白的基因,这些基因在STEMI中高度表达。我们通过ELISA验证了40名STEMI和32名健康受试者中这10种假定的生物标志物的血液蛋白表达水平。数据表明,PGLYRP1,IRAK3和VNN3比传统的CK-MB或肌钙蛋白对STEMI具有更高的特异性和敏感性。ACS的血液转录组扫描证明了STEMI的早期分子标记。在这里,我们报告了一种新颖的生物标记物,可通过简单的ELISA方法在医院急诊室诊断STEMI。

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