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姿势性心动过速综合征患者的自身免疫性 IgG。

Autoimmunoreactive IgGs from patients with postural orthostatic tachycardia syndrome.

机构信息

Department of Internal Medicine, Mayo Clinic, Rochester, MN 55905, USA.

出版信息

Proteomics Clin Appl. 2012 Dec;6(11-12):615-25. doi: 10.1002/prca.201200049. Epub 2012 Nov 8.

Abstract

PURPOSE

Autoantibodies are implicated in the pathogenesis of cardiovascular diseases and cardiac arrhythmias. In this pilot study, we tested the hypothesis that autoantibodies are present in patients with postural orthostatic tachycardia syndrome (POTS).

EXPERIMENTAL DESIGN

Seven control subjects (6 F:1 M, average age 36.1 years) and ten patients with the diagnosis of POTS (7 F: 3 M, average age 35.1 years) provided informed consent and 30 mL of venous blood. Human heart membrane proteins were resolved by 2DE and immunoblotted against purified IgGs from controls and patients.

RESULTS

Eighteen protein spots immunoreactive specifically against patient IgGs were detected and they were excised from gels, trypsin-digested, and analyzed by nanoLC-electrospray MS/MS. Forty unique proteins were identified and these include proteins that are associated with cardiac hypertrophy (mimecan, myozenin), cardiac remodeling (periostin), cardiomyopathy (desmin, desmoplakin), cell survival (laminin), structural integrity (filamin), chaperone proteins (crystalline, HSP70), mitochondrial enzymes, and channel proteins. Ingenuity Pathway Analysis showed multiple pathways were involved including those that regulate energy metabolism, redox, fibrosis, cardiac hypertrophy, and degeneration.

CONCLUSIONS AND CLINICAL RELEVANCE

Autoantibodies are present in patients with POTS. These autoantibodies cross-react with a wide range of cardiac proteins and may induce alterations in cardiac function. Autoimmune pathogenetic mechanisms should be further explored in these patients.

摘要

目的

自身抗体与心血管疾病和心律失常的发病机制有关。在这项初步研究中,我们检验了这样一个假设,即体位性心动过速综合征(POTS)患者存在自身抗体。

实验设计

7 名对照受试者(6 女 1 男,平均年龄 36.1 岁)和 10 名 POTS 患者(7 女 3 男,平均年龄 35.1 岁)同意并提供 30 毫升静脉血。通过 2-DE 分离人心脏膜蛋白,并与对照和患者的纯化 IgG 进行免疫印迹。

结果

检测到 18 个与患者 IgG 特异性反应的蛋白质斑点,将其从凝胶中切下,胰蛋白酶消化,并通过纳升 LC-电喷雾 MS/MS 进行分析。鉴定出 40 个独特的蛋白质,其中包括与心脏肥大(mimecan,myozenin)、心脏重构(periostin)、心肌病(desmin,desmoplakin)、细胞存活(laminin)、结构完整性(filamin)、伴侣蛋白(crystalline,HSP70)、线粒体酶和通道蛋白相关的蛋白质。Ingenuity Pathway Analysis 显示,多个途径被涉及,包括调节能量代谢、氧化还原、纤维化、心脏肥大和退化的途径。

结论和临床相关性

POTS 患者存在自身抗体。这些自身抗体与广泛的心脏蛋白发生交叉反应,可能导致心脏功能改变。应在这些患者中进一步探讨自身免疫发病机制。

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