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MALDI 成像鉴定出肠型胃癌中具有预后价值的七种新型组织标志物蛋白的特征。

MALDI imaging identifies prognostic seven-protein signature of novel tissue markers in intestinal-type gastric cancer.

机构信息

Institute of Pathology, Helmholtz Zentrum München-German Research Center for Environmental Health, Neuherberg, Germany.

出版信息

Am J Pathol. 2011 Dec;179(6):2720-9. doi: 10.1016/j.ajpath.2011.08.032. Epub 2011 Oct 18.

Abstract

Proteomics-based approaches allow us to investigate the biology of cancer beyond genomic initiatives. We used histology-based matrix-assisted laser desorption/ionization (MALDI) imaging mass spectrometry to identify proteins that predict disease outcome in gastric cancer after surgical resection. A total of 181 intestinal-type primary resected gastric cancer tissues from two independent patient cohorts were analyzed. Protein profiles of the discovery cohort (n = 63) were directly obtained from tumor tissue sections by MALDI imaging. A seven-protein signature was associated with an unfavorable overall survival independent of major clinical covariates. The prognostic significance of three individual proteins identified (CRIP1, HNP-1, and S100-A6) was validated immunohistochemically on tissue microarrays of an independent validation cohort (n = 118). Whereas HNP-1 and S100-A6 were found to further subdivide early-stage (Union Internationale Contre le Cancer [UICC]-I) and late-stage (UICC II and III) cancer patients into different prognostic groups, CRIP1, a protein previously unknown in gastric cancer, was confirmed as a novel and independent prognostic factor for all patients in the validation cohort. The protein pattern described here serves as a new independent indicator of patient survival complementing the previously known clinical parameters in terms of prognostic relevance. These results show that this tissue-based proteomic approach may provide clinically relevant information that might be beneficial in improving risk stratification for gastric cancer patients.

摘要

基于蛋白质组学的方法使我们能够在超越基因组学计划的层面上研究癌症生物学。我们使用基于组织学的基质辅助激光解吸/电离(MALDI)成像质谱法来鉴定在胃癌手术后预测疾病结局的蛋白质。总共分析了来自两个独立患者队列的 181 例肠型原发性胃癌组织。通过 MALDI 成像直接从肿瘤组织切片中获取发现队列(n = 63)的蛋白质谱。与主要临床协变量无关,一个由七种蛋白质组成的特征与不良的总生存率相关。在独立验证队列(n = 118)的组织微阵列上通过免疫组织化学验证了三个单独鉴定的蛋白质(CRIP1、HNP-1 和 S100-A6)的预后意义。虽然 HNP-1 和 S100-A6 被发现进一步将早期(国际抗癌联盟[UICC]-I)和晚期(UICC II 和 III)癌症患者细分为不同的预后组,但 CRIP1 是胃癌中以前未知的蛋白质,被确认为验证队列中所有患者的新的独立预后因素。这里描述的蛋白质模式是一种新的独立的患者生存指标,补充了先前在预后相关性方面已知的临床参数。这些结果表明,这种基于组织的蛋白质组学方法可以提供临床相关的信息,可能有助于改善胃癌患者的风险分层。

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