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以免疫性血小板减少性紫癜(ITP)作为模型疾病,通过基于质谱的抗体介导自身抗原鉴定(MS-AMIDA)来鉴定新型自身抗原。

Identification of novel autoantigens via mass spectroscopy-based antibody-mediated identification of autoantigens (MS-AMIDA) using immune thrombocytopenic purpura (ITP) as a model disease.

作者信息

Kamhieh-Milz Julian, Sterzer Viktor, Celik Hatice, Khorramshahi Omid, Fadl Hassan Moftah Reham, Salama Abdulgabar

机构信息

Charité University Medicine Berlin, Institute of Transfusion Medicine, Robert-Koch Platz 3, 10115 Berlin, Germany.

Charité University Medicine Berlin, Institute of Transfusion Medicine, Robert-Koch Platz 3, 10115 Berlin, Germany.

出版信息

J Proteomics. 2017 Mar 22;157:59-70. doi: 10.1016/j.jprot.2017.01.012. Epub 2017 Jan 27.

DOI:10.1016/j.jprot.2017.01.012
PMID:28137667
Abstract

Immune thrombocytopenic purpura (ITP) is one of the best characterized autoimmune diseases. Autoantibodies (AABs) against platelet antigens are considered as the diagnostic hallmark of ITP, but are detectable in only 50% of patients. We designed and applied a novel proteomic approach termed Mass Spectroscopy-based Antibody-Mediated Identification of Autoantigens (MS-AMIDA) for platelet antigens. Patients were separated into patients with classical AABs [ITP(+)] and patients without AABs [ITP(-)]. Altogether, 181 potential AAGs were found in ITP(+) and 135 AAGs in ITP(-), with 34 and 23 AAGs reproducibly found in two runs of MS-AMIDA. After subtracting identifiers from the controls, 57 AAGs in ITP(+) and 29 AAGs in ITP(+) remained, with 16 AAGs commonly found in ITP(+) and ITP(-) patients. Label-free quantification (LFQ) revealed 15 potential AAGs that are quantitatively stronger in ITP. Dot blot validation was performed on hexokinase 1 (HK1), E1 pyruvate dehydrogenase (E1-PDH), coagulation factor XIII, filamin A (FLNA), non-muscle myosin 9. Eleven patients were found to have anti-HK1 AABs, one patient had anti-E1-PDH AABs, and two patients had anti-FLNA AABs. Most antigens were of intracellular origin with significant association with actin-cytoskeleton and regulation of programmed cell death. In conclusion, novel AAGs for ITP were identified using MS-AMIDA.

摘要

免疫性血小板减少性紫癜(ITP)是特征最为明确的自身免疫性疾病之一。抗血小板抗原的自身抗体(AABs)被视为ITP的诊断标志,但仅在50%的患者中可检测到。我们设计并应用了一种名为基于质谱的自身抗原抗体介导鉴定法(MS-AMIDA)的新型蛋白质组学方法来鉴定血小板抗原。患者被分为具有经典AABs的患者[ITP(+)]和没有AABs的患者[ITP(-)]。总共,在ITP(+)患者中发现了181种潜在的自身抗原(AAGs),在ITP(-)患者中发现了135种AAGs,其中有34种和23种AAGs在两轮MS-AMIDA中均可重复检测到。从对照中减去标识符后,ITP(+)患者中剩下57种AAGs,ITP(-)患者中剩下29种AAGs,其中有16种AAGs在ITP(+)和ITP(-)患者中均常见。无标记定量(LFQ)显示有15种潜在的AAGs在ITP中定量表达更强。对己糖激酶1(HK1)、E1丙酮酸脱氢酶(E1-PDH)、凝血因子XIII、细丝蛋白A(FLNA)、非肌肉肌球蛋白9进行了斑点印迹验证。发现11名患者有抗HK1 AABs,1名患者有抗E1-PDH AABs,2名患者有抗FLNA AABs。大多数抗原起源于细胞内,与肌动蛋白细胞骨架和程序性细胞死亡的调节密切相关。总之,使用MS-AMIDA鉴定出了ITP的新型AAGs。

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