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靶向胶内 MRM:一种用于人类粪便中结直肠癌生物标志物发现的假设驱动方法。

Targeted in-gel MRM: a hypothesis driven approach for colorectal cancer biomarker discovery in human feces.

机构信息

Ludwig Institute for Cancer Research, Melbourne Tumour Biology Branch, The University of Melbourne, Melbourne, Australia.

出版信息

J Proteome Res. 2010 Sep 3;9(9):4346-55. doi: 10.1021/pr100509e.

Abstract

Colorectal cancer (CRC) is the second most common cause of cancer-related deaths in both men and women. The fecal occult blood test is currently the first line method for CRC screening but has an unacceptably low sensitivity and specificity. Improved screening tests are therefore urgently required for early stage CRC screening. We have described a hypothesis-driven approach for a rapid biomarker discovery process whereby selected proteins previously implicated as colorectal cancer-associated proteins (CCAP), which can potentially be shed into the feces from a colorectal tumor, are targeted for excision from 1D-SDS-PAGE based on their predicted molecular weight followed by directed identification and relative quantification using multiple reaction monitoring (MRM). This approach can significantly reduce the time for clinical assay development with the added advantage that many proteins will have been validated by previous in vitro and/or in vivo studies. Sixty potential CCAPs were selected from the literature and appropriate MRM conditions were established for measurement of proteotypic peptides. Nineteen of these proteins were detected in the feces from a patient with colorectal cancer. Relative quantitation of these 19 CCAP across 5 CRC patients and 5 healthy volunteers were carried out, revealing hemoglobin, myeloperoxidase, S100A9, filamin A and l-plastin to be present only in the feces of CRC patients.

摘要

结直肠癌(CRC)是男性和女性癌症相关死亡的第二大常见原因。粪便潜血试验是目前 CRC 筛查的首选方法,但敏感性和特异性均不令人满意。因此,迫切需要改进的筛查试验来进行早期 CRC 筛查。我们描述了一种基于假设的快速生物标志物发现过程,该过程针对先前被认为与结直肠癌相关的蛋白质(CCAP),这些蛋白质可能从结直肠肿瘤中脱落到粪便中,根据其预测的分子量,从 1D-SDS-PAGE 上靶向切除,然后使用多重反应监测(MRM)进行定向鉴定和相对定量。这种方法可以显著缩短临床检测方法的开发时间,并且具有许多蛋白质已经通过先前的体外和/或体内研究得到验证的额外优势。从文献中选择了 60 种潜在的 CCAP,并为测量蛋白质肽建立了适当的 MRM 条件。在一位结直肠癌患者的粪便中检测到其中 19 种蛋白质。对 5 例 CRC 患者和 5 名健康志愿者的这些 19 种 CCAP 进行相对定量,结果显示血红蛋白、髓过氧化物酶、S100A9、细丝蛋白 A 和 l-肌动蛋白仅存在于 CRC 患者的粪便中。

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