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诊断子痫前期的血清肽的肽组学鉴定

Peptidomic Identification of Serum Peptides Diagnosing Preeclampsia.

作者信息

Wen Qiaojun, Liu Linda Y, Yang Ting, Alev Cantas, Wu Shuaibin, Stevenson David K, Sheng Guojun, Butte Atul J, Ling Xuefeng B

机构信息

Department of Surgery, Stanford University, Stanford, California, United States of America.

出版信息

PLoS One. 2013 Jun 19;8(6):e65571. doi: 10.1371/journal.pone.0065571. Print 2013.

DOI:10.1371/journal.pone.0065571
PMID:23840341
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3686758/
Abstract

We sought to identify serological markers capable of diagnosing preeclampsia (PE). We performed serum peptide analysis (liquid chromatography mass spectrometry) of 62 unique samples from 31 PE patients and 31 healthy pregnant controls, with two-thirds used as a training set and the other third as a testing set. Differential serum peptide profiling identified 52 significant serum peptides, and a 19-peptide panel collectively discriminating PE in training sets (n = 21 PE, n = 21 control; specificity = 85.7% and sensitivity = 100%) and testing sets (n = 10 PE, n = 10 control; specificity = 80% and sensitivity = 100%). The panel peptides were derived from 6 different protein precursors: 13 from fibrinogen alpha (FGA), 1 from alpha-1-antitrypsin (A1AT), 1 from apolipoprotein L1 (APO-L1), 1 from inter-alpha-trypsin inhibitor heavy chain H4 (ITIH4), 2 from kininogen-1 (KNG1), and 1 from thymosin beta-4 (TMSB4). We concluded that serum peptides can accurately discriminate active PE. Measurement of a 19-peptide panel could be performed quickly and in a quantitative mass spectrometric platform available in clinical laboratories. This serum peptide panel quantification could provide clinical utility in predicting PE or differential diagnosis of PE from confounding chronic hypertension.

摘要

我们试图鉴定能够诊断子痫前期(PE)的血清学标志物。我们对来自31例PE患者和31例健康孕妇对照的62份独特样本进行了血清肽分析(液相色谱质谱法),其中三分之二用作训练集,另外三分之一用作测试集。差异血清肽谱分析鉴定出52种显著的血清肽,一个由19种肽组成的组合在训练集(n = 21例PE,n = 21例对照;特异性 = 85.7%,敏感性 = 100%)和测试集(n = 10例PE,n = 10例对照;特异性 = 80%,敏感性 = 100%)中均能有效区分PE。该组合中的肽来自6种不同的蛋白质前体:13种来自纤维蛋白原α(FGA),1种来自α-1抗胰蛋白酶(A1AT),1种来自载脂蛋白L1(APO-L1),1种来自间α胰蛋白酶抑制剂重链H4(ITIH4),2种来自激肽原-1(KNG1),1种来自胸腺素β-4(TMSB4)。我们得出结论,血清肽能够准确区分活动性PE。在临床实验室可用的定量质谱平台上,可以快速进行19种肽组合的检测。这种血清肽组合定量检测在预测PE或从混淆的慢性高血压中鉴别诊断PE方面具有临床应用价值。

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