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一种利用角质层活检鉴定银屑病生物标志物的蛋白质组学方法。

A proteomics approach to the identification of biomarkers for psoriasis utilising keratome biopsy.

机构信息

Department of Biochemistry and Molecular Biology, University of Southern Denmark, Campusvej 55, Odense DK-5230, Denmark.

出版信息

J Proteomics. 2013 Dec 6;94:176-85. doi: 10.1016/j.jprot.2013.09.010. Epub 2013 Sep 20.

Abstract

UNLABELLED

The discovery of plasma biomarkers for psoriasis vulgaris may aid clinicians in disease grading and monitoring of treatment response. We have therefore developed a proteomics/mass spectrometry based workflow which enables biomarker discovery from psoriasis patient samples. We have utilised keratome skin biopsy, which results in reduced cellular complexity compared to punch biopsy. Furthermore, we applied short term ex vivo culture in order to enrich for a "secretome" sub-proteome reflective of the disease and enriched in potential biomarkers. Using these sample preparation techniques we performed a quantitative proteomics screen of four patients with psoriasis using stable isotope dimethyl labelling and identified over 50 proteins consistently altered in abundance in psoriasis lesional versus non-lesional skin. This includes several canonical psoriasis related proteins (e.g. S100A7 [Psoriasin] and FABP5 [Epidermal Fatty Acid Binding Protein]) and more than 30 novel alterations. From this disease localised dataset we further assessed several proteins as potential biomarkers in the plasma of patients with psoriasis versus healthy controls utilising selected reaction monitoring mass spectrometry (SRM-MS/MS).

BIOLOGICAL SIGNIFICANCE

The significance of this study for proteome research in psoriasis and dermal disease is threefold. 1) A novel sample preparation method for isolation of dermal proteomes enriched in extracellular proteins is described, which may be of interest to other researchers in the field. 2) Novel psoriasis associated alterations in protein abundance are described at the disease site, bolstering knowledge in an area dominated by transcript level studies and 3) Profilin 1 is described as a candidate plasma biomarker of psoriasis, this is of value in itself and it proves that our workflow can yield results in terms of biomarker discovery.

摘要

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寻常型银屑病的血浆生物标志物的发现可能有助于临床医生对疾病进行分级和监测治疗反应。因此,我们开发了一种基于蛋白质组学/质谱的工作流程,可从银屑病患者样本中发现生物标志物。我们利用了角质层皮肤活检,与穿刺活检相比,这减少了细胞复杂性。此外,我们还进行了短期的离体培养,以富集反映疾病的“分泌组”亚蛋白组,并富集潜在的生物标志物。使用这些样本制备技术,我们对 4 名寻常型银屑病患者进行了稳定同位素二甲基标记的定量蛋白质组学筛选,发现银屑病病变与非病变皮肤相比,有 50 多种蛋白质的丰度发生了一致的改变。这包括几种典型的银屑病相关蛋白(如 S100A7[Psoriasin]和 FABP5[表皮脂肪酸结合蛋白])和 30 多种新的改变。从这个疾病局部数据集,我们进一步利用选择反应监测质谱(SRM-MS/MS)评估了几种蛋白质作为银屑病患者与健康对照者血浆中的潜在生物标志物。

生物学意义

这项研究对银屑病和皮肤疾病蛋白质组学的意义有三点。1)描述了一种新的分离富含细胞外蛋白的皮肤蛋白质组的样本制备方法,这可能对该领域的其他研究人员有兴趣。2)描述了疾病部位新的与银屑病相关的蛋白质丰度改变,这增强了在以转录水平研究为主的领域的知识。3)描述了原肌球蛋白 1 是银屑病的候选血浆生物标志物,这本身就很有价值,并且证明了我们的工作流程能够在发现生物标志物方面取得成果。

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