Free Fatty Acids in CSF and Neurological Clinical Scores: Prognostic Value for Stroke Severity in ICU.

IF 1.8 Q3 CRITICAL CARE MEDICINE Critical Care Research and Practice Pub Date : 2020-07-17 eCollection Date: 2020-01-01 DOI:10.1155/2020/5808129
Sayed Gaber, Sherine Ibrahim ElGazzar, Mahmoud Qenawi, Nora Ismail Mohamed Abbas
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引用次数: 1

Abstract

Introduction: Brain ischemia initiated significant increase in FFAs in animal studies. Accumulation of FFA can lead to liberation of inflammatory byproducts that contribute to neuronal death. Increased risk of systemic thromboembolism was seen in animal models after FFA infusion possibly through activation of factor XII by stearic acids. The clinical studies that examined the relation between stroke in humans and CSF biomarkers are infrequent. Aim of Work. We tried to evaluate the potential role of FFAs in CSF in the diagnosis and the prognosis of ICU patients with AIS while comparing the results to traditional neurological scoring systems. Patients and Methods. Our study included 80 patients who were admitted to ICU with acute ischemic stroke (AIS) within 24 hours of the onset of cerebral infarction. CSF samples were obtained at admission. The FFA levels were measured using the sensitive enzyme-based colorimetric method. The NIHSS, GCS, and mRS were evaluated at admission and at 30 days. Univariate and multivariate analysis were used to evaluate the stroke outcome according to FFA levels in CSF.

Results: Worsening of the GCS (<7) at 30 days showed a significant correlation with FFA in CSF. The ROC curve showed a cutoff value of 0.27 nmol/µl, sensitivity of 62.9%, and specificity of 72.2%. There was a significant correlation between FFA in CSF and the mRS >2 at 30 days. The ROC curve showed a cutoff value of 0.27 nmol/µl, specificity of 69.2%, and sensitivity of 59.7%. There was a significant correlation between FFA in CSF and the NIHSS ≥ 16 at 30 days. The ROC curve showed a cutoff value of 0.27 nmol/µl, specificity of 72.2%, and sensitivity of 62.9%. Our study subdivided patients according to infarction volume and compared the 2 subgroups with FFA in CSF. We found a significant difference between 2 subgroups. FFA levels showed a positive correlation with infarction volume ≥145 ml. The ROC curve showed a cutoff value of 0.25 nmol/µl, sensitivity of 76.9%, and specificity of 71.4%. Our study showed that FFA in CSF was a significant predictor of all-cause mortality (0.37 + 0.26, P value 0.007). The ROC curve showed a cutoff value of 0.27, specificity of 72.2%, and sensitivity of 62.9%. There was a positive correlation between FFA in CSF and neurological causes of mortality (0.48 + 0.38, P value 0.037). The ROC curve showed a cutoff value of 0.37 nmol/µl, specificity of 76.1%, and sensitivity of 61.5%.

Conclusion: FFA in CSF may serve as an independent prognostic biomarker for assessing the prognosis of acute ischemic stroke and the clinical outcome. It might be a useful biomarker for early detection of high-risk patients for poor outcome and hence more aggressive treatment.

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脑脊液游离脂肪酸与神经学临床评分:对ICU中风严重程度的预后价值。
在动物实验中,脑缺血引起FFAs显著增加。游离脂肪酸的积累可导致炎性副产物的释放,从而导致神经元死亡。在动物模型中观察到FFA输注后全身性血栓栓塞的风险增加,可能是通过硬脂酸激活因子XII。检验人类中风与脑脊液生物标志物之间关系的临床研究并不多见。工作目标。我们试图评估脑脊液FFAs在AIS ICU患者诊断和预后中的潜在作用,并将结果与传统神经学评分系统进行比较。患者和方法。我们的研究纳入了80例在脑梗死发病24小时内入院的急性缺血性卒中(AIS)患者。入院时采集脑脊液样本。采用灵敏的酶比色法测定FFA水平。入院时和入院30天分别评估NIHSS、GCS和mRS。采用单因素和多因素分析,根据脑脊液中FFA水平评估脑卒中结局。结果:GCS(µl)恶化,敏感性为62.9%,特异性为72.2%。30 d时脑脊液FFA与mRS >2有显著相关性。ROC曲线截断值为0.27 nmol/µl,特异性为69.2%,敏感性为59.7%。30 d时脑脊液FFA与NIHSS≥16有显著相关性。ROC曲线截断值为0.27 nmol/µl,特异性为72.2%,敏感性为62.9%。我们的研究根据梗死体积对患者进行细分,并比较两个亚组脑脊液中的FFA。我们发现两个亚组之间存在显著差异。FFA水平与梗死体积≥145 ml呈正相关。ROC曲线的截止值为0.25 nmol/µl,灵敏度为76.9%,特异性为71.4%。我们的研究显示脑脊液中的FFA是全因死亡率的重要预测因子(0.37 + 0.26,P值0.007)。ROC曲线截断值为0.27,特异性为72.2%,敏感性为62.9%。脑脊液中FFA与神经学死亡原因呈正相关(0.48 + 0.38,P值0.037)。ROC曲线截断值为0.37 nmol/µl,特异性为76.1%,敏感性为61.5%。结论:脑脊液FFA可作为评估急性缺血性脑卒中预后和临床转归的独立预后生物标志物。它可能是一种有用的生物标志物,用于早期发现预后不良的高危患者,从而进行更积极的治疗。
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来源期刊
Critical Care Research and Practice
Critical Care Research and Practice CRITICAL CARE MEDICINE-
CiteScore
3.60
自引率
0.00%
发文量
34
审稿时长
14 weeks
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