首页> 外文期刊>The journal of maternal-fetal & neonatal medicine >Isobaric labeling and tandem mass spectrometry: a novel approach for profiling and quantifying proteins differentially expressed in amniotic fluid in preterm labor with and without intra-amniotic infection/inflammation.
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Isobaric labeling and tandem mass spectrometry: a novel approach for profiling and quantifying proteins differentially expressed in amniotic fluid in preterm labor with and without intra-amniotic infection/inflammation.

机译:等压标记和串联质谱法:一种新的方法,用于分析和定量在有或没有羊水感染/炎症的早产中羊水中差异表达的蛋白质。

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OBJECTIVE: Examination of the amniotic fluid (AF) proteome has been previously attempted to identify useful biomarkers in predicting the outcome of preterm labor (PTL). Isobaric Tag for Relative and Absolute Quantitation (iTRAQ) labeling allows direct ratiometric comparison of relative abundance of identified protein species among multiplexed samples. The purpose of this study was to apply, for the first time, the combination of iTRAQ and tandem mass spectrometry to identify proteins differentially regulated in AF samples of women with spontaneous PTL and intact membranes with and without intra-amniotic infection/inflammation (IAI). METHODS: A cross-sectional study was designed and included AF samples from patients with spontaneous PTL and intact membranes in the following groups: (1) patients without IAI who delivered at term (n = 26); (2) patients who delivered preterm without IAI (n = 25); and (3) patients with IAI (n = 24). Proteomic profiling of AF samples was performed using a workflow involving tryptic digestion, iTRAQ labeling and multiplexing, strong cation exchange fractionation, and liquid chromatography tandem mass spectrometry. Twenty-five separate 4-plex samples were prepared and analyzed. RESULTS: Collectively, 123,011 MS(2) spectra were analyzed, and over 25,000 peptides were analyzed by database search (X!Tandem and Mascot), resulting in the identification of 309 unique high-confidence proteins. Analysis of differentially present iTRAQ reporter peaks revealed many proteins that have been previously reported to be associated with preterm delivery with IAI. Importantly, many novel proteins were found to be up-regulated in the AF of patients with PTL and IAI including leukocyte elastase precursor, Thymosin-like 3, and 14-3-3 protein isoforms. Moreover, we observed differential expression of proteins in AF of patients who delivered preterm in the absence of IAI in comparison with those with PTL who delivered at term including Mimecan precursor, latent-transforming growth factor beta-binding protein isoform 1L precursor, and Resistin. These findings have been confirmed for Resistin in an independent cohort of samples using ELISA. Gene ontology enrichment analysis was employed to reveal families of proteins participating in distinct biological processes. We identified enrichment for host defense, anti-apoptosis, metabolism/catabolism and cell and protein mobility, localization and targeting. CONCLUSIONS: (1) Proteomics with iTRAQ labeling is a profiling tool capable of revealing differential expression of proteins in AF; (2) We discovered 82 proteins differentially expressed in three clinical subgroups of premature labor, 67 which were heretofore unknown. Of particular importance is the identification of proteins differentially expressed in AF from women who delivered preterm in the absence of IAI. This is the first report of the positive identification of biomarkers in this subgroup of patients.
机译:目的:以前曾尝试对羊水(AF)蛋白质组进行检查,以鉴定有用的生物标志物,以预测早产(PTL)的结果。相对定量和绝对定量(iTRAQ)标记的等压标记允许对多重样品之间鉴定的蛋白质种类的相对丰度进行直接比率比较。这项研究的目的是首次将iTRAQ和串联质谱法结合使用,以鉴定具有和不具有羊水内感染/炎症(IAI)的自发性PTL和完整膜的女性AF样品中差异调节的蛋白质。 。方法:设计了一项横断面研究,包括以下组的自发性PTL和完整膜患者的AF样品:(1)足月分娩的无IAI患者(n = 26); (2)早产而无IAI的患者(n = 25); (3)IAI患者(n = 24)。使用包括胰蛋白酶消化,iTRAQ标记和多路复用,强阳离子交换分级分离和液相色谱串联质谱在内的工作流程进行AF样品的蛋白质组分析。制备并分析了二十五个分开的4-plex样品。结果:总共分析了123,011 MS(2)光谱,并通过数据库搜索(X!Tandem和Mascot)分析了25,000多种肽,从而鉴定出309种独特的高可信度蛋白。对存在差异的iTRAQ报告基因峰的分析揭示了许多以前被报道与IAI早产有关的蛋白质。重要的是,发现许多新蛋白在PTL和IAI患者的房颤中被上调,包括白细胞弹性蛋白酶前体,胸腺素样3和14-3-3蛋白同工型。此外,我们观察到与未足月分娩的PTL患者相比,在没有IAI的情况下分娩的早产患者房颤中蛋白质的差异表达包括Mimecan前体,潜在转化生长因子β结合蛋白同工型1L前体和Resistin。使用ELISA在独立的样本队列中已确认了Resistin的这些发现。基因本体富集分析被用来揭示参与不同生物学过程的蛋白质家族。我们确定了宿主防御,抗凋亡,代谢/分解代谢以及细胞和蛋白质迁移,定位和靶向的富集。结论:(1)带有iTRAQ标记的蛋白质组学是一种能够揭示AF中蛋白质差异表达的分析工具。 (2)我们在早产的三个临床亚组中发现了82种差异表达的蛋白质,迄今未知的有67种。尤为重要的是鉴定在没有IAI的情况下进行早产的妇女在房颤中差异表达的蛋白质。这是该患者亚组中生物标志物阳性鉴定的首次报道。

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