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首页> 外文期刊>Journal of Translational Medicine >Fibrosis independent atrial fibrillation in older patients is driven by substrate leukocyte infiltration: diagnostic and prognostic implications to patients undergoing cardiac surgery
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Fibrosis independent atrial fibrillation in older patients is driven by substrate leukocyte infiltration: diagnostic and prognostic implications to patients undergoing cardiac surgery

机译:纤维化的老年患者的独立心房颤动由底物白细胞浸润驱动:对经过心脏手术的患者的诊断和预后影响

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BACKGROUND:The objectives of the study were to characterize and quantify cellular inflammation and structural remodeling of human atria and correlate findings with molecular markers of inflammation and patient surrogate outcome.METHODS:Voluntary participants undergoing heart surgery were enrolled in the study and blood samples were collected prior to surgery, and right atrium samples were harvested intraoperatively. Blood samples were analyzed by flow cytometry and complete blood counts. Atrial samples were divided for fixed fibrosis analysis, homogenized for cytokine analysis and digested for single cell suspension flow cytometry.RESULTS:A total of 18 patients were enrolled and samples assessed. Isolated cells from the atria revealed a CD45+ population of ~?20%, confirming a large number of leukocytes. Further characterization revealed this population as 57% lymphocytes and 26% monocyte/macrophages (MoΦ), with the majority of the latter cells being classical (CD14++/CD16-). Interstitial fibrosis was present in 87% of samples and correlated significantly with patient age. Older patients (?65) had significantly more atrial fibrosis and cellular inflammation. AFib patients had no distinguishing feature of atrial fibrosis and had significantly greater CD45+ MoΦ, increased expression of MMP9 and presented with a significant correlation in length of stay to CCL-2/MCP-1 and NLR (neutrophil-to-lymphocyte ratio).CONCLUSION:Atrial fibrosis is correlated with age and not determinate to AFib. However, severity of atrial leukocyte infiltration and markers of matrix degradation are determinant to AFib. This also correlated with CCL2 (or MCP-1) and NLR-indicative of marked inflammation. These data show the potential importance of diagnostic and prognostic assessments that could inform clinical decision making in regard to the intensity of AFib patient management.
机译:背景:该研究的目的是表征和量化人类阿里亚人的细胞炎症和结构重塑,并与炎症和患者代理结果的分子标记相关结果。方法:志愿参与者接受心脏病的志愿参与者在研究中,收集血液样本在手术之前,术中收获右中庭样品。通过流式细胞术分析血样并完全血液计数。对心房样品分为固定纤维化分析,均质化细胞因子分析并消化为单细胞悬浮流量细胞学。结果:注册了18名患者并评估样品。来自Atria的分离细胞显示CD45 +〜20%的群体,确认了大量的白细胞。进一步表征揭示了这种群体为57%的淋巴细胞和26%单核细胞/巨噬细胞(MOΦ),其中大多数后一细胞是经典的(CD14 ++ / CD16-)。在87%的样品中存在间质纤维化,并随患者年龄显着相关。年龄较大的患者(>β65)具有显着更多的心房纤维化和细胞炎症。 AFIB患者没有区别特征性心房纤维化,并且具有明显更大的CD45 +MOφ,MMP9的表达增加,并在保持CCL-2 / MCP-1和NLR(中性粒细胞 - 淋巴细胞比率)中具有显着的相关性。结论:心房纤维化与年龄相关,而不是确定AFIB。然而,心房白细胞浸润的严重程度和基质降解标记是AFIB的决定因素。这也与CCL2(或MCP-1)和NLR指示有关标记炎症的相关性。这些数据表明诊断和预后评估的潜在重要性,可以在临床决策方面通向AFIB患者管理的强度。

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