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Plasma Lipid Profiling Identifies Biomarkers of Cerebral Microvascular Disease

机译:血浆脂质谱分析确定脑微血管疾病的生物标志物

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摘要

Brain-specific sphingolipids (SLs) may serve as effective biomarkers of white matter hyperintensities (WMH). Here, we investigate the efficacy of SLs as a novel fluid-based biomarker to identify WMH reflective of chronic ischemia. Patients presenting to our stroke center for evaluation of acute neurological deficits were enrolled in the Advanced Serum Profiling in Recent Stroke (ASPIRE) study. From this cohort of 202 individuals, 58 patients who underwent an MRI and did not have a clinical stroke event were included in this study. Plasma samples were collected at the time of MRI, and targeted SL profiling was performed by HPLC/tandem mass spectrometry. T2 FLAIR imaging was evaluated for WMH and scored according to the Fazekas scoring (FS) method and manually quantified. Twenty two SLs were definitively identified, consisting of ceramide (Cer) and sphingomyelin (SM) species. Of these, two sphingolipids, SM 38:1 and Cer 34:1, significantly correlated with high FS (r = 0.287, p = 0.029, and r = 0.356, p = 0.006, respectively) and were used in subsequent analysis. SM 38:1 (OR 1.129, 95% CI 1.032, 1.236, p = 0.008) and Cer 34:1 (OR 1.118, 95% CI 1.031, 1.212, p = 0.007), accurately differentiated between FS 0–2 vs. 2.5–6 in regression analysis. A combined lipid score demonstrated fair discrimination in ROC analysis (AUC = 0.729, p = 0.003) and was cross-validated using leave-one-out analysis. Plasma levels of brain-specific SLs may serve as effective biomarkers of subacute white matter disease.
机译:脑特异性鞘脂(SLs)可以作为白质高信号(WMH)的有效生物标志物。在这里,我们调查SLs作为一种新型的基于液体的生物标记物的功效,以识别反映慢性缺血的WMH。到我们的卒中中心评估急性神经功能缺损的患者参加了“近期卒中高级血清分析”(ASPIRE)研究。该研究共纳入202名患者,其中58例接受了MRI检查且未发生临床中风事件。在MRI时收集血浆样品,并通过HPLC /串联质谱进行靶向SL分析。对T2 FLAIR成像进行WMH评估,并根据Fazekas评分(FS)方法进行评分并手动量化。最终确定了22个SL,其中包括神经酰胺(Cer)和鞘磷脂(SM)物种。其中,两种鞘脂SM 38:1和Cer 34:1与高FS显着相关(分别为r = 0.287,p = 0.029,r = 0.356,p = 0.006),并用于后续分析。 SM 38:1(OR 1.129,95%CI 1.032,1.236,p = 0.008)和Cer 34:1(OR 1.118,95%CI 1.031,1.212,p = 0.007),FS 0-2与2.5之间精确区分–6进行回归分析。组合脂质评分在ROC分析中显示出公平的歧视性(AUC = 0.729,p = 0.003),并使用留一法分析进行了交叉验证。脑特异性SL的血浆水平可以作为亚急性白质病的有效生物标志物。

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