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人类胃液蛋白质组学的特征分析揭示了不同 pH 值依赖性的蛋白质谱:对生物标志物研究的影响。

Characterization of the human gastric fluid proteome reveals distinct pH-dependent protein profiles: implications for biomarker studies.

机构信息

Division of Medical Sciences, Humphrey Oei Institute of Cancer Research, National Cancer Centre , Singapore.

出版信息

J Proteome Res. 2011 Oct 7;10(10):4535-46. doi: 10.1021/pr200349z. Epub 2011 Sep 22.

DOI:10.1021/pr200349z
PMID:21842849
Abstract

Gastric fluid is a source of gastric cancer biomarkers. However, very little is known about the normal gastric fluid proteome and its biological variations. In this study, we performed a comprehensive analysis of the human gastric fluid proteome using samples obtained from individuals with benign gastric conditions. Gastric fluid proteins were prefractionated using ultracentrifuge filters (3 kDa cutoff) and analyzed by two-dimensional gel electrophoresis (2-DE) and multidimensional LC-MS/MS. Our 2-DE analysis of 170 gastric fluid samples revealed distinct protein profiles for acidic and neutral samples, highlighting pH effects on protein composition. By 2D LC-MS/MS analysis of pooled samples, we identified 284 and 347 proteins in acidic and neutral samples respectively (FDR ≤1%), of which 265 proteins (72.4%) overlapped. However, unlike neutral samples, most proteins in acidic samples were identified from peptides in the filtrate (i.e., <3 kDa). Consistent with this finding, immunoblot analysis of six potential gastric cancer biomarkers rarely detected full-length proteins in acidic samples. These findings have important implications for biomarker studies because a majority of gastric cancer patients have neutral gastric fluid compared to noncancer controls. Consequently, sample stratification, choice of proteomic approaches, and validation strategy can profoundly affect the interpretation of biomarker findings. These observations should help to refine gastric fluid biomarker studies.

摘要

胃液是胃癌生物标志物的来源。然而,对于正常胃液蛋白质组及其生物学变化,我们知之甚少。在这项研究中,我们使用来自良性胃部疾病个体的样本,对人类胃液蛋白质组进行了全面分析。使用超滤器(3 kDa 截止值)对胃液蛋白质进行预分级,并用二维凝胶电泳(2-DE)和多维 LC-MS/MS 进行分析。我们对 170 个胃液样本的 2-DE 分析显示酸性和中性样本具有明显不同的蛋白质图谱,突出了 pH 对蛋白质组成的影响。通过对混合样本的 2D LC-MS/MS 分析,我们分别在酸性和中性样本中鉴定出 284 种和 347 种蛋白质(FDR ≤1%),其中 265 种蛋白质(72.4%)重叠。然而,与中性样本不同,酸性样本中的大多数蛋白质都是从滤液(即 <3 kDa)中的肽鉴定出来的。与这一发现一致的是,对六种潜在胃癌生物标志物的免疫印迹分析很少在酸性样本中检测到全长蛋白质。这些发现对生物标志物研究具有重要意义,因为与非癌症对照相比,大多数胃癌患者的胃液呈中性。因此,样本分层、蛋白质组学方法的选择和验证策略可以极大地影响生物标志物发现的解释。这些观察结果应该有助于完善胃液生物标志物研究。

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