Identification of Differentially-Expressed Proteins between Early Submucosal Non-Invasive and Invasive Colorectal Cancer Using 2D-DIGE and Mass Spectrometry

J. Zhang; M-Q. Song; J-S. Zhu; Z. Zhou; Z-P. Xu; W-X. Chen; N-W. Chen

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Identification of Differentially-Expressed Proteins between Early Submucosal Non-Invasive and Invasive Colorectal Cancer Using 2D-DIGE and Mass Spectrometry

机译：使用2D-DIGE和质谱法鉴定早期黏膜下非浸润性和浸润性结直肠癌之间差异表达的蛋白质

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Early detection and diagnosis of colorectal cancer (CRC) are closely related to a better therapeutic outcome, and the five-year survival rate of early CRC is over 90%. Though endoscopic minimally invasive treatment has become a quick and effective therapy for early CRC, endoscopic biopsies are usually not deep enough to obtain tissues from the submucosal layer and it is difficult to determine whether early CRC has infiltrated into the submucosa. Therefore, in the present study, we constructed tumor models of early submucosal non-invasive CRC (SNICRC) and submucosal invasive CRC (SICRC) in Fischer-344 rats induced by N-methyl-N-nitrosourea (MNU). The differentially-expressed proteins were analyzed and identified in SNICRC, SICRC and normal control (NC) tissues using highly sensitive two-dimensional differential gel electrophoresis (2D-DIGE) coupled with mass spectrometry (MS). Proteomic data revealed 132 protein spots between SNICRC and SICRC, 162 protein spots between SICRC and NC and 154 protein spots between SNICRC and NC which were found differentially expressed. These differential spots were picked, in-gel digested and peptide mass fingerprints were obtained by MALDI-TOF-MS/MS. Finally, five differentially-expressed proteins in SNICRC, SICRC and NC were identified, and increases in Transgelin, peptidylprolyl isomerase A (PPIA) and tropomyosin alpha isoform d were observed, while decreases in carbonic anhydrase 2 (CAII) and an unnamed protein were detected in SICRC compared with SNICRC and NC. Furthermore, Fluorescence-based quantitative polymerase chain reaction (FQ-PCR), Western blotting and immunohistochemistry assays also revealed significant upregulation of Transgelin expression and down-regulation of CAII expression in SICRC tissues. In conclusion, 2D-DIGE is confirmed to be an efficient strategy that enables us to identify differentially-expressed proteins between early SNICRC and SICRC. The potential biomarkers such as Transgelin and CAII may be used for the detection of early SICRC

机译：大肠癌（CRC）的早期发现和诊断与更好的治疗效果密切相关，早期CRC的五年生存率超过90％。尽管内镜微创治疗已成为早期CRC的快速有效疗法，但内镜活检通常不够深，无法从粘膜下层获得组织，因此很难确定早期CRC是否已渗透到粘膜下层。因此，在本研究中，我们构建了N-甲基-N-亚硝基脲（MNU）诱导的Fischer-344大鼠早期黏膜下非侵入性CRC（SNICRC）和黏膜下侵入性CRC（SICRC）的肿瘤模型。使用高灵敏度的二维差分凝胶电泳（2D-DIGE）和质谱（MS）对SNICRC，SICRC和正常对照（NC）组织中的差异表达蛋白进行分析和鉴定。蛋白质组学数据显示SNICRC和SICRC之间有132个蛋白点，SICRC和NC之间有162个蛋白点，SNICRC和NC之间有154个蛋白点，它们被差异表达。挑选这些差异点，进行凝胶消化，并通过MALDI-TOF-MS / MS获得肽质量指纹图。最后，在SNICRC，SICRC和NC中鉴定了5种差异表达的蛋白质，观察到Transgelin，肽基脯氨酰异构酶A（PPIA）和原肌球蛋白α亚型d的增加，而碳酸酐酶2（CAII）和未命名的蛋白质的减少。 SICRC与SNICRC和NC相比。此外，基于荧光的定量聚合酶链反应（FQ-PCR），Western印迹和免疫组织化学分析还显示出SICRC组织中Transgelin表达的显着上调和CAII表达的下调。总之，已确认2D-DIGE是一种有效的策略，使我们能够识别早期SNICRC和SICRC之间差异表达的蛋白质。潜在的生物标志物，如转基因蛋白和CAII可用于早期SICRC的检测

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《International journal of immunopathology and pharmacology.》 |2011年第4期|共11页
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J. Zhang; M-Q. Song; J-S. Zhu; Z. Zhou; Z-P. Xu; W-X. Chen; N-W. Chen;
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Identification of Differentially-Expressed Proteins between Early Submucosal Non-Invasive and Invasive Colorectal Cancer Using 2D-DIGE and Mass Spectrometry

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