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在严重依赖血管活性药物的急性心力衰竭中,循环生物标志物对药物治疗与机械循环支持的反应

Circulating biomarker responses to medical management vs. mechanical circulatory support in severe inotrope-dependent acute heart failure.

作者信息

Meredith Anna J, Dai Darlene L Y, Chen Virginia, Hollander Zsuzsanna, Ng Raymond, Kaan Annemarie, Tebbutt Scott, Ramanathan Krishnan, Cheung Anson, McManus Bruce M

机构信息

Department of Pathology and Laboratory MedicineUniversity of British ColumbiaVancouverCanada; PROOF Centre of ExcellenceVancouverCanada.

PROOF Centre of Excellence Vancouver Canada.

出版信息

ESC Heart Fail. 2016 Jun;3(2):86-96. doi: 10.1002/ehf2.12076. Epub 2015 Nov 24.

DOI:10.1002/ehf2.12076
PMID:27774271
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5063158/
Abstract

BACKGROUND

Severe inotrope-dependent acute heart failure (AHF) is associated with poor clinical outcomes. There are currently no well-defined blood biomarkers of response to treatment that can guide management or identify recovery in this patient population. In the present study, we characterized the levels of novel and emerging circulating biomarkers of heart failure in patients with AHF over the first 30 days of medical management or mechanical circulatory support (MCS). We hypothesized a shared a plasma proteomic treatment response would be identifiable in both patient groups, representing reversal of the AHF phenotype.

METHODS AND RESULTS

Time course plasma samples of the first 30 days of therapy, obtained from patients managed medically ( = 8) or with implantable MCS ( = 5), underwent semi-targeted and candidate biomarker analyses, using multiple reaction monitoring (MRM) mass spectrometry, antibody arrays, and enzyme-linked immunosorbent assays. Differentially expressed proteins were identified using robust limma for MRM and antibody array data. Patients managed medically or with implantable MCS had a shared proteomic signature of six plasma proteins: circulating cardiotrophin 1, cardiac troponin T, clusterin, and dickopff 1 increased, while levels of C-reactive protein and growth differentiation factor 15 decreased in both groups over the 30 day time course.

CONCLUSIONS

We have characterized the temporal proteomic signature of clinical recovery in AHF patients managed medically or with MCS, over the first 30 days of treatment. Changes in biomarker expression over the time course of treatment may provide a basis for understanding the biological basis of AHF, potentially identifying novel markers and pathophysiologic mechanisms of recovery.

摘要

背景

严重依赖血管活性药物的急性心力衰竭(AHF)与不良临床结局相关。目前尚无明确的治疗反应血液生物标志物可指导该患者群体的管理或确定其恢复情况。在本研究中,我们对接受药物治疗或机械循环支持(MCS)的AHF患者在治疗的前30天内新型和新兴的循环心力衰竭生物标志物水平进行了特征分析。我们假设在两个患者组中都可识别出共同的血浆蛋白质组治疗反应,这代表AHF表型的逆转。

方法与结果

从接受药物治疗(n = 8)或植入式MCS治疗(n = 5)的患者中获取治疗前30天的时间进程血浆样本,使用多反应监测(MRM)质谱、抗体阵列和酶联免疫吸附测定进行半靶向和候选生物标志物分析。使用稳健的limma软件对MRM和抗体阵列数据进行差异表达蛋白的鉴定。接受药物治疗或植入式MCS治疗的患者有六种血浆蛋白的共同蛋白质组特征:循环心肌营养素1、心肌肌钙蛋白T、簇集蛋白和Dickkopf 1增加,而两组在30天的时间进程中C反应蛋白和生长分化因子15的水平均下降。

结论

我们已经描述了接受药物治疗或MCS治疗的AHF患者在治疗的前30天内临床恢复的时间蛋白质组特征。治疗过程中生物标志物表达的变化可能为理解AHF的生物学基础提供依据,有可能识别新的标志物和恢复的病理生理机制。

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