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Stromal proteome expression profile and muscle-invasive bladder cancer research

机译:基质蛋白质组表达谱和肌肉浸润性膀胱癌的研究

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Background To globally characterize the cancer stroma expression profile of muscle-invasive transitional cell carcinoma and to discuss the cancer biology as well as biomarker discovery from stroma. Laser capture micro dissection was used to harvest purified muscle-invasive bladder cancer stromal cells and normal urothelial stromal cells from 4 paired samples. Two-dimensional liquid chromatography tandem mass spectrometry was used to identify the proteome expression profile. The differential proteins were further analyzed using bioinformatics tools and compared with the published literature. Results We identified 868/872 commonly expressed proteins and 978 differential proteins from 4 paired cancer and normal stromal samples using laser capture micro dissection coupled with two-dimensional liquid chromatography tandem mass spectrometry. 487/491 proteins uniquely expressed in cancerormal stroma. Differential proteins were compared with the entire list of the international protein index (IPI), and there were 42/42 gene ontology (GO) terms exhibited as enriched and 8/5 exhibited as depleted in cellular Component, respectively. Significantly altered pathways between cancerormal stroma mainly include metabolic pathways, ribosome, focal adhesion, etc. Finally, descriptive statistics show that the stromal proteins with extremes of PI and MW have the same probability to be a biomarker. Conclusions Based on our results, stromal cells are essential component of the cancer, biomarker discovery and network based multi target therapy should consider neoplastic cells itself and corresponding stroma as whole one.
机译:背景技术要全面表征肌肉浸润性移行细胞癌的癌基质表达谱,并讨论癌生物学以及从基质中发现生物标志物的方法。激光捕获显微解剖用于从4对样本中收集纯化的浸润性肌肉浸润性膀胱癌基质细胞和正常尿路上皮基质细胞。二维液相色谱串联质谱法用于鉴定蛋白质组表达谱。使用生物信息学工具进一步分析了差异蛋白,并与已发表的文献进行了比较。结果我们使用激光捕获显微解剖结合二维液相色谱串联质谱法从4个配对的癌症和正常基质样品中鉴定出868/872共同表达的蛋白质和978个差异蛋白质。在癌症/正常基质中独特表达的487/491蛋白。将差异蛋白质与国际蛋白质索引(IPI)的整个列表进行比较,并且在细胞组分中分别有42/42个基因本体论(GO)术语表现为富集,而8/5表现为耗尽。癌症/正常基质之间的途径发生了显着改变,主要包括代谢途径,核糖体,粘着斑等。最后,描述性统计数据显示,具有PI和MW极值的基质蛋白具有相同的生物标志物可能性。结论根据我们的结果,基质细胞是癌症的重要组成部分,基于生物标志物的发现和基于网络的多靶点治疗应将肿瘤细胞本身和相应的基质视为一个整体。

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