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使用18O标记的差异膜蛋白质组学来鉴定胆管癌的生物标志物。

Differential membrane proteomics using 18O-labeling to identify biomarkers for cholangiocarcinoma.

作者信息

Kristiansen Troels Zakarias, Harsha H C, Grønborg Mads, Maitra Anirban, Pandey Akhilesh

机构信息

McKusick-Nathans Institute of Genetic Medicine and Department of Biological Chemistry, Johns Hopkins University, Baltimore, Maryland 21205, USA.

出版信息

J Proteome Res. 2008 Nov;7(11):4670-7. doi: 10.1021/pr800215n. Epub 2008 Oct 8.

DOI:10.1021/pr800215n
PMID:18839982
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3204659/
Abstract

Quantitative proteomic methodologies allow profiling of hundreds to thousands of proteins in a high-throughput fashion. This approach is increasingly applied to cancer biomarker discovery to identify proteins that are differentially regulated in cancers. Fractionation of protein samples based on enrichment of cellular subproteomes prior to mass spectrometric analysis can provide increased coverage of certain classes of molecules. We used a membrane protein enrichment strategy coupled with 18O labeling based quantitative proteomics to identify proteins that are highly expressed in cholangiocarcinomas. In addition to identifying several proteins previously known to be overexpressed in cholangiocarcinoma, we discovered a number of molecules that were previously not associated with cholangiocarcinoma. Using immunoblotting and immunohistochemical labeling of tissue microarrays, we validated Golgi membrane protein 1, Annexin IV and Epidermal growth factor receptor pathway substrate 8 (EPS8) as candidate biomarkers for cholangiocarcinomas. Golgi membrane protein 1 was observed to be overexpressed in 89% of cholangiocarcinoma cases analyzed by staining tissue microarrays. In light of recent reports showing that Golgi membrane protein 1 is detectable in serum, further investigation into validation of this protein has the potential to provide a biomarker for early detection of cholangiocarcinomas.

摘要

定量蛋白质组学方法能够以高通量方式对成百上千种蛋白质进行分析。这种方法越来越多地应用于癌症生物标志物的发现,以识别在癌症中差异调节的蛋白质。在质谱分析之前,基于细胞亚蛋白质组的富集对蛋白质样品进行分级分离,可以增加对某些类分子的覆盖范围。我们使用了一种膜蛋白富集策略,并结合基于18O标记的定量蛋白质组学来鉴定在胆管癌中高表达的蛋白质。除了鉴定出几种先前已知在胆管癌中过表达的蛋白质外,我们还发现了一些先前与胆管癌无关的分子。通过对组织微阵列进行免疫印迹和免疫组织化学标记,我们验证了高尔基体膜蛋白1、膜联蛋白IV和表皮生长因子受体途径底物8(EPS8)作为胆管癌的候选生物标志物。通过对组织微阵列进行染色分析,在89%的胆管癌病例中观察到高尔基体膜蛋白1过表达。鉴于最近有报道显示血清中可检测到高尔基体膜蛋白1,对该蛋白进行进一步验证研究有可能为胆管癌的早期检测提供一种生物标志物。

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