Sawa Kostin, Manfred Richter, Florian Krizanic, Benjamin Sasko Sasko, Theodoros Kelesidis, Nikolaos Pagonas
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We used immunolabeling for CD45, CD66b and CD11b for (N) and citrullinated histone3 (citH3), peptidylarginine deiminase-4 (PAD-4), neutrophil elastase (NE) and myeoloperoxidase (MPO) for NETosis. These proteins were investigated also by quantitative fluorescence intensity analysis, Western blot and quantitative polymerase chain reaction (qPCR).\nResults. Compared to control, the number of N was increased 3-4 fold in HF. We found that using a single marker for NETosemarkers, 43.2% of N in DCM, 46.7% in ICM and 57.3% in infCMP experienced NETosis. The use of double labeling (NE with CitH3) showed that 55.6% (47.2-60.9) of N developed NETosis in DCM, 57.9% (52.2-64.8) in ICM and 79.4% (71.1-84.9) in infCMP. The difference between the N who underwent NETosis in infCMP and those in DCM was statistically different (p<0.01). The proportion of N who developed NETosis or formed NETs in control tissue was less than 5% and differed significantly from that in HF patients, regardless of etiology (p<0.01). These results were confirmed by quantitative fluorescence analysis, Western blot and qPCR.\nConclusions: This is the first study to show the occurrence of NETosis in human hearts in situ indicating that NETosis is an important component of low-grade myocardial inflammation in HF.","PeriodicalId":501297,"journal":{"name":"medRxiv - Cardiovascular Medicine","volume":null,"pages":null},"PeriodicalIF":0.0000,"publicationDate":"2024-07-10","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"NETosis is an important component of chronic inflammation in patients with heart failure\",\"authors\":\"Sawa Kostin, Manfred Richter, Florian Krizanic, Benjamin Sasko Sasko, Theodoros Kelesidis, Nikolaos Pagonas\",\"doi\":\"10.1101/2024.07.09.24310187\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"Background and aim. We have previously demonstrated that heart failure (HF) is characterized by low-grade myocardial inflammation. However, the role of neutrophils (N), neutrophil extracellular traps (NETs) and neutrophil cell death by NETosis in the myocardium of patients with HF remains largely unknown. The present study investigated the number of neutrophils (N) and their proportion undergoing NETosis and developing NETs in HF.\\nMethods. We used quantitative confocal microscopy and NETosis markers in the left ventricular biopsies obtained from 5 control and from patients with HF due to dilated (DCM, n=7), inflammatory (infCMP, n=7) and ischemic cardiomyopathy (ICM, n=7). We used immunolabeling for CD45, CD66b and CD11b for (N) and citrullinated histone3 (citH3), peptidylarginine deiminase-4 (PAD-4), neutrophil elastase (NE) and myeoloperoxidase (MPO) for NETosis. 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引用次数: 0
摘要
背景和目的。我们以前曾证实,心力衰竭(HF)以低度心肌炎症为特征。然而,嗜中性粒细胞(N)、嗜中性粒细胞胞外捕获物(NET)和嗜中性粒细胞NETosis导致的嗜中性粒细胞死亡在心力衰竭患者心肌中的作用在很大程度上仍然未知。本研究调查了心房颤动患者中性粒细胞(N)的数量及其发生NETosis和NETs的比例。我们使用定量共聚焦显微镜和NETosis标记物对5名对照组和因扩张型(DCM,n=7)、炎症型(infCMP,n=7)和缺血性心肌病(ICM,n=7)导致的HF患者的左心室活检组织进行了检测。我们使用 CD45、CD66b 和 CD11b 免疫标记法检测(N),使用瓜氨酸组蛋白 3(citH3)、肽精氨酸脱氨酶-4(PAD-4)、中性粒细胞弹性蛋白酶(NE)和麦芽过氧化物酶(MPO)免疫标记法检测 NETosis。还通过荧光强度定量分析、Western 印迹和定量聚合酶链反应(qPCR)对这些蛋白质进行了研究。与对照组相比,高频患者的 N 数量增加了 3-4 倍。我们发现,使用单一标记物作为 NETosemarkers,43.2% 的 DCM、46.7% 的 ICM 和 57.3% 的 infCMP N 出现 NETosis。使用双重标记(NE 与 CitH3)显示,DCM 中 55.6% (47.2-60.9)的 N 出现 NETosis,ICM 中 57.9% (52.2-64.8),infCMP 中 79.4%(71.1-84.9)。在 infCMP 中接受 NETosis 的 N 与在 DCM 中接受 NETosis 的 N 之间存在统计学差异(p<0.01)。在对照组织中发生 NETosis 或形成 NET 的 N 所占比例低于 5%,与高频患者相比,无论病因如何,均有显著差异(p<0.01)。这些结果得到了荧光定量分析、Western blot 和 qPCR 的证实:这是首次在人体心脏原位发现NETosis的研究,表明NETosis是HF低度心肌炎症的重要组成部分。
NETosis is an important component of chronic inflammation in patients with heart failure
Background and aim. We have previously demonstrated that heart failure (HF) is characterized by low-grade myocardial inflammation. However, the role of neutrophils (N), neutrophil extracellular traps (NETs) and neutrophil cell death by NETosis in the myocardium of patients with HF remains largely unknown. The present study investigated the number of neutrophils (N) and their proportion undergoing NETosis and developing NETs in HF.
Methods. We used quantitative confocal microscopy and NETosis markers in the left ventricular biopsies obtained from 5 control and from patients with HF due to dilated (DCM, n=7), inflammatory (infCMP, n=7) and ischemic cardiomyopathy (ICM, n=7). We used immunolabeling for CD45, CD66b and CD11b for (N) and citrullinated histone3 (citH3), peptidylarginine deiminase-4 (PAD-4), neutrophil elastase (NE) and myeoloperoxidase (MPO) for NETosis. These proteins were investigated also by quantitative fluorescence intensity analysis, Western blot and quantitative polymerase chain reaction (qPCR).
Results. Compared to control, the number of N was increased 3-4 fold in HF. We found that using a single marker for NETosemarkers, 43.2% of N in DCM, 46.7% in ICM and 57.3% in infCMP experienced NETosis. The use of double labeling (NE with CitH3) showed that 55.6% (47.2-60.9) of N developed NETosis in DCM, 57.9% (52.2-64.8) in ICM and 79.4% (71.1-84.9) in infCMP. The difference between the N who underwent NETosis in infCMP and those in DCM was statistically different (p<0.01). The proportion of N who developed NETosis or formed NETs in control tissue was less than 5% and differed significantly from that in HF patients, regardless of etiology (p<0.01). These results were confirmed by quantitative fluorescence analysis, Western blot and qPCR.
Conclusions: This is the first study to show the occurrence of NETosis in human hearts in situ indicating that NETosis is an important component of low-grade myocardial inflammation in HF.
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