在ICU的COVID-19阳性成人中,血清神经丝光升高,并与合并症心血管疾病、神经系统并发症和疾病敏锐度相关。

Cardiology and cardiovascular medicine Pub Date : 2021-10-01 Epub Date: 2021-10-13 DOI:10.26502/fccm.92920221
Meredith Hay, Lee Ryan, Matthew Huentelman, John Konhilas, Christina Hoyer-Kimura, Thomas G Beach, Geidy E Serrano, Eric M Reiman, Kaj Blennow, Henrik Zetterberg, Sairam Parthasarathy
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引用次数: 7

摘要

在重症新冠肺炎患者中,长期神经系统后果的风险才刚刚开始被认识到。尽管最近的研究表明,重症新冠肺炎患者的神经系统结构性损伤增加,但对新冠肺炎神经损伤与新冠肺炎患者全身炎症疾病的关系知之甚少。这项试点观察性研究的目的是检查入住重症监护室(ICU)的新冠肺炎阳性患者的血清神经丝轻蛋白(NfL,一种神经元损伤的测量方法)与共病心血管疾病(CVD)和神经并发症之间的关系。在这项针对2020年4月至8月期间入住亚利桑那州图森市ICU的100名患者的观察性研究中,89名患者新冠肺炎呈阳性(新冠肺炎阳性),11名患者呈新冠肺炎阴性(新冠病毒阴性)。对健康对照组(n=8)进行检查以进行比较。主要结果和测量是受试者的人口统计学、血清NfL、CVD的存在和程度、糖尿病、连续器官衰竭评估评分(SOFA)、神经并发症的存在以及血液化学小组数据。与新冠肺炎阴性ICU患者(19.3±5.6 pg/ml)相比,ICU中的新冠肺炎阳性患者的平均Nfl水平(229.6±163 pg/ml)显著更高,Welch t检验,p=0.01,健康对照组(12.3±3.1 pg/ml),Welch t检验,p=0.005。在伴有心血管疾病和糖尿病的患者中,COVID阳性ICU患者的Nfl水平显著较高(n=35,log Nfl 1.6±.09),并与较高的SOFA评分相关(r=.5,p=.001)。这些发现表明,在严重的新冠肺炎疾病中,通过系统性心血管疾病和外周炎症的水平。了解这些新冠肺炎幸存者全身炎症性疾病对中枢神经变性的贡献,对于设计预防长期神经和认知功能障碍的介入疗法至关重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Serum Neurofilament Light is elevated in COVID-19 Positive Adults in the ICU and is associated with Co-Morbid Cardiovascular Disease, Neurological Complications, and Acuity of Illness.

Serum Neurofilament Light is elevated in COVID-19 Positive Adults in the ICU and is associated with Co-Morbid Cardiovascular Disease, Neurological Complications, and Acuity of Illness.

Serum Neurofilament Light is elevated in COVID-19 Positive Adults in the ICU and is associated with Co-Morbid Cardiovascular Disease, Neurological Complications, and Acuity of Illness.

Serum Neurofilament Light is elevated in COVID-19 Positive Adults in the ICU and is associated with Co-Morbid Cardiovascular Disease, Neurological Complications, and Acuity of Illness.

In critically ill COVID-19 patients, the risk of long-term neurological consequences is just beginning to be appreciated. While recent studies have identified that there is an increase in structural injury to the nervous system in critically ill COVID-19 patients, there is little known about the relationship of COVID-19 neurological damage to the systemic inflammatory diseases also observed in COVID-19 patients. The purpose of this pilot observational study was to examine the relationships between serum neurofilament light protein (NfL, a measure of neuronal injury) and co-morbid cardiovascular disease (CVD) and neurological complications in COVID-19 positive patients admitted to the intensive care unit (ICU). In this observational study of one-hundred patients who were admitted to the ICU in Tucson, Arizona between April and August 2020, 89 were positive for COVID-19 (COVID-pos) and 11 was COVID-negative (COVID-neg). A healthy control group (n=8) was examined for comparison. The primary outcomes and measures were subject demographics, serum NfL, presence and extent of CVD, diabetes, sequential organ failure assessment score (SOFA), presence of neurological complications, and blood chemistry panel data. COVID-pos patients in the ICU had significantly higher mean levels of Nfl (229.6 ± 163 pg/ml) compared to COVID-neg ICU patients (19.3 ± 5.6 pg/ml), Welch's t-test, p =.01 and healthy controls (12.3 ± 3.1 pg/ml), Welch's t-test p =.005. Levels of Nfl in COVID-pos ICU patients were significantly higher in patients with concomitant CVD and diabetes (n=35, log Nfl 1.6±.09), and correlated with higher SOFA scores (r=.5, p =.001). These findings suggest that in severe COVID-19 disease, the central neuronal and axonal damage in these patients may be driven, in part, by the level of systemic cardiovascular disease and peripheral inflammation. Understanding the contributions of systemic inflammatory disease to central neurological degeneration in these COVID-19 survivors will be important to the design of interventional therapies to prevent long-term neurological and cognitive dysfunction.

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