Seraph 100 Hemoperfusion for Management of Severe COVID-19: Assessment of Serum and Plasma Analytes Pre- and Post-Filtration.

IF 2.2 3区 医学 Q3 HEMATOLOGY Blood Purification Pub Date : 2024-12-11 DOI:10.1159/000542995
Michael Rouse, Eric R Gann, Joost Brandsma, Victor A Sugiharto, Henry Robertson, Pavol Genzor, Hua-Wei Chen, Mark P Simons, Seth A Schobel, Josh G Chenoweth, Sarah A Jenkins, Danielle V Clark, Jeffrey Della Volpe, Stephen Chitty, Ian M Rivera, Michael Lewis, Caroline Park, Amay Parikh, Pooja Vir, Ian J Stewart, Kathleen P Pratt
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Abstract

Introduction: We report an Intervention/outcome study of 33 severe COVID-19 subjects who received Seraph 100 Microbind Affinity Blood Filter (Seraph 100) hemoperfusion therapy (15 survivors, 18 non-survivors) under emergency authorization from the FDA. Our objective was to determine if Seraph 100 hemoperfusion reduces SARS-CoV-2 RNA titers and/or markers of inflammation and/or epi/endothelial damage.

Methods: Viral RNA and 78 protein analytes related to endothelial/epithelial damage and/or inflammation were quantified in systemic blood samples from 33 severe COVID-19 subjects collected upon intensive care unit (ICU) admission and then immediately before and after blood passed through the heparin-based Seraph 100 filter at two time points on the first day of hemoperfusion. Viral RNA titers were quantified using droplet digital PCR. Protein analytes were quantified using multiplex/multi-analyte panels on MesoScale Discovery and ProteinSimple Ella platforms.

Results: A total of 15/33 subjects had detectable viral RNA in baseline samples (shortly after ICU admission). These initial viremia levels were low, and they did not change uniformly post-perfusion. Five of 55 protein analytes that were upregulated 1.4-120X at ICU admission relative to healthy controls showed significant decreases across the filter during the indicated time points on the first day of hemoperfusion: IP-10/CXCL10, fms-like tyrosine kinase 1, MIG/CXCL9, hepatocyte growth factor (HGF), and receptor for advanced glycosylation end products (RAGE). Paired t tests identified 25 additional analytes that showed significant decreases (p < 0.05) only without Bonferroni correction.

Conclusion: Initial freely circulating SARS-CoV-2 RNA levels of ICU-admitted subjects were low or undetectable. The Seraph 100 filter did not significantly reduce viral RNA titers in their plasma. However, multiple circulating proteins with roles in inflammation, endothelial/epithelial damage, and/or angiogenesis decreased significantly across the filter. Larger prospective trials will be required to determine if such transient reductions translate into improved patient outcomes. However, this study did not demonstrate a direct reduction of free SARS-CoV-2 viral RNA by the Seraph 100.

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Seraph-100血液灌流治疗重症COVID-19:过滤前后血清和血浆分析物的评估
我们报告了一项干预/结局研究,33名重症COVID-19患者接受了FDA紧急授权的Seraph100 Microbind亲和血液过滤器(Seraph 100)血液灌流治疗(15名幸存者,18名非幸存者)。我们的目的是确定Seraph 100血液灌流是否会降低SARS-CoV-2 RNA滴度和/或炎症和/或内皮细胞损伤的标志物。a方法对33例重症COVID-19患者在ICU入院时以及血液灌流第一天的两个时间点,在血液通过基于肝素的Seraph 100过滤器之前和之后采集的全身血液样本进行病毒RNA和78种与内皮/上皮损伤和/或炎症相关的蛋白质分析。采用微滴数字PCR定量检测病毒RNA滴度。在MesoScale Discovery和ProteinSimple-Ella平台上使用多重/多重分析面板对蛋白质分析进行定量。结果15/33例患者(入院后不久)在基线样本中检测到病毒RNA。这些初始病毒血症水平较低,灌注后不均匀变化。在ICU入院时,55种蛋白分析物中有5种相对于健康对照上调1.4-120X,在血液灌流第一天的指定时间点,整个滤过物的IP-10/CXCL10、fms样酪氨酸激酶(Flt-1)、MIG/CXCL9、肝细胞生长因子(HGF)和晚期糖基化终产物受体(RAGE)显著降低。配对t检验确定了另外25个分析物显示显著降低(p
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来源期刊
Blood Purification
Blood Purification 医学-泌尿学与肾脏学
CiteScore
5.80
自引率
3.30%
发文量
69
审稿时长
6-12 weeks
期刊介绍: Practical information on hemodialysis, hemofiltration, peritoneal dialysis and apheresis is featured in this journal. Recognizing the critical importance of equipment and procedures, particular emphasis has been placed on reports, drawn from a wide range of fields, describing technical advances and improvements in methodology. Papers reflect the search for cost-effective solutions which increase not only patient survival but also patient comfort and disease improvement through prevention or correction of undesirable effects. Advances in vascular access and blood anticoagulation, problems associated with exposure of blood to foreign surfaces and acute-care nephrology, including continuous therapies, also receive attention. Nephrologists, internists, intensivists and hospital staff involved in dialysis, apheresis and immunoadsorption for acute and chronic solid organ failure will find this journal useful and informative. ''Blood Purification'' also serves as a platform for multidisciplinary experiences involving nephrologists, cardiologists and critical care physicians in order to expand the level of interaction between different disciplines and specialities.
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