In-depth characterization of the secretome of colorectal cancer metastatic cells identifies key proteins in cell adhesion, migration, and invasion

BarderasR.; MendesM.; TorresS.; BartoloméR.A.; López-LucendogM.; Villar-VázquezR.; Peláez-GarcíaA.; FuenteE.; BonillaF.; CasalJ.I.

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In-depth characterization of the secretome of colorectal cancer metastatic cells identifies key proteins in cell adhesion, migration, and invasion

机译：大肠癌转移细胞分泌基因组的深入表征鉴定了细胞粘附，迁移和侵袭中的关键蛋白

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Liver metastasis in colorectal cancer is the major cause of cancer-related deaths. To identify and characterize proteins associated with colon cancer metastasis, we have compared the conditioned serum-free medium of highly metastatic KM12SM colorectal cancer cells with the parental, poorly metastatic KM12C cells using quantitative stable isotope labeling by amino acids in cell culture (SILAC) analyses on a linear ion trap-Orbitrap Velos mass spectrometer. In total, 1337 proteins were simultaneously identified in SILAC forward and reverse experiments. For quantification, 1098 proteins were selected in both experiments, with 155 proteins showing >1.5-fold change. About 52% of these proteins were secreted directly or using alternative secretion pathways. GDF15, S100A8/A9, and SERPINI1 showed capacity to discriminate cancer serum samples from healthy controls using ELISAs. In silico analyses of deregulated proteins in the secretome of metastatic cells showed a major abundance of proteins involved in cell adhesion, migration, and invasion. To characterize the tumorigenic and metastatic properties of some top up- and down-regulated proteins, we used siRNA silencing and antibody blocking. Knockdown expression of NEO1, SERPINI1, and PODXL showed a significant effect on cellular adhesion. Silencing or blocking experiments with SOSTDC1, CTSS, EFNA3, CD137L/ TNFSF9, ZG16B, and Midkine caused a significant decrease in migration and invasion of highly metastatic cells. In addition, silencing of SOSTDC1, EFNA3, and CD137L/TNFSF9 reduced liver colonization capacity of KM12SM cells. Finally, the panel of six proteins involved in invasion showed association with poor prognosis and overall survival after dataset analysis of gene alterations. In summary, we have defined a collection of proteins that are relevant for understanding the mechanisms underlying adhesion, migration, invasion, and metastasis in colorectal cancer.

机译：大肠癌中的肝转移是与癌症相关的死亡的主要原因。为了鉴定和表征与结肠癌转移相关的蛋白质，我们使用细胞培养物中的氨基酸进行定量稳定同位素标记，比较了高度转移性KM12SM结直肠癌细胞的条件化无血清培养基与亲代性，转移性较差的KM12C细胞。在线性离子阱Orbitrap Velos质谱仪上在SILAC正向和反向实验中，总共鉴定出1337种蛋白质。为了定量，在两个实验中选择了1098个蛋白质，其中155个蛋白质显示> 1.5倍的变化。这些蛋白质中约有52％是直接分泌或通过其他分泌途径分泌的。 GDF15，S100A8 / A9和SERPINI1显示了使用ELISA区分健康对照和癌症血清样品的能力。在计算机分析中，转移细胞分泌基因组中失调的蛋白质的分析表明，大量蛋白质参与细胞粘附，迁移和侵袭。为了表征某些上调和下调蛋白的致瘤和转移特性，我们使用了siRNA沉默和抗体阻断。 NEO1，SERPINI1和PODXL的组合表达显示出对细胞粘附的显着影响。用SOSTDC1，CTSS，EFNA3，CD137L / TNFSF9，ZG16B和Midkine进行的沉默或阻断实验导致高度转移细胞的迁移和侵袭显着降低。此外，SOSTDC1，EFNA3和CD137L / TNFSF9的沉默降低了KM12SM细胞的肝脏定殖能力。最后，在对基因改变进行数据集分析后，涉及入侵的六种蛋白质组显示出不良的预后和总体存活率。总而言之，我们定义了一组蛋白质，这些蛋白质与了解结肠直肠癌中黏附，迁移，侵袭和转移的机制有关。

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《Molecular & cellular proteomics: MCP》 |2013年第6期|共19页
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BarderasR.; MendesM.; TorresS.; BartoloméR.A.; López-LucendogM.; Villar-VázquezR.; Peláez-GarcíaA.; FuenteE.; BonillaF.; CasalJ.I.;
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1. In-depth characterization of the secretome of colorectal cancer metastatic cells identifies key proteins in cell adhesion, migration, and invasion [J] . BarderasR., MendesM., TorresS., Molecular & cellular proteomics: MCP . 2013,第6期

机译：大肠癌转移细胞分泌基因组的深入表征鉴定了细胞粘附，迁移和侵袭中的关键蛋白
2. Inositol hexaphosphate (IP6) inhibits key events of cancer metastasis: I. In vitro studies of adhesion, migration and invasion of MDA-MB 231 human breast cancer cells. [J] . Tantivejkul K, Vucenik I, Shamsuddin AM Anticancer Research: International Journal of Cancer Research and Treatment . 2003,第5Appa期

机译：六磷酸肌醇（IP6）抑制癌症转移的关键事件：I. MDA-MB 231人乳腺癌细胞粘附，迁移和侵袭的体外研究。
3. alpha-Tubulin Acetylation Elevated in Metastatic and Basal-like Breast Cancer Cells Promotes Microtentacle Formation, Adhesion, and Invasive Migration [J] . Boggs Amanda E., Vitolo Michele I., Whipple Rebecca A., Cancer research: The official organ of the American Association for Cancer Research, Inc . 2015,第1期

机译：转移和基底样乳腺癌细胞中的α-Tubulin乙酰化升高促进微触手的形成，粘附和侵袭性迁移。
4. Single Cell Genomic Profiling of Circulating Tumor Cells (CTCs) from Metastatic Colorectal Cancer (mCRC) Identify Tumor Heterogeneity and Rare Somatic Driver Alterations [C] . Stephanie Greene, Angel Rodriguez, Jerry Lee, International Molecular Medicine Tri-Conference. . 2016

机译：转移结直肠癌（MCRC）的循环肿瘤细胞（CTC）的单细胞基因组分析识别肿瘤异质性和稀有躯体驾驶员改变
5. Comparative Analysis on Innate Immune System Function in Metastatic Breast, Colorectal, and Prostate Cancer Patients with Circulating Tumor Cells [D] . Santos, Mark Anthony Francisco. 2014

机译：转移性乳腺癌，结直肠癌和前列腺癌患者循环肿瘤细胞先天免疫系统功能的比较分析
6. In-depth Characterization of the Secretome of Colorectal Cancer Metastatic Cells Identifies Key Proteins in Cell Adhesion Migration and Invasion [O] . Rodrigo Barderas, Marta Mendes, Sofia Torres, 2013

机译：大肠癌转移细胞分泌蛋白的深入表征鉴定了细胞粘附迁移和侵袭中的关键蛋白。
7. In-depth Characterization of the Secretome of Colorectal Cancer Metastatic Cells Identifies Key Proteins in Cell Adhesion, Migration, and Invasion [O] . Rodrigo Barderas, Marta Mendes, Sofia Torres, 2013

机译：结肠直肠癌转移细胞的沉淀的深度表征鉴定了细胞粘附，迁移和侵袭中的关键蛋白质
8. Transcription Factor Stat5, A Novel Therapeutic Protein, Inhibits Metastatic Potential and Invasive Characteristics of Human Breast Cancer Cells [R] . Sultan, A. S. 2004

机译：转录因子stat5，一种新型治疗蛋白，抑制转移潜能和人乳腺癌细胞的侵袭特征

In-depth characterization of the secretome of colorectal cancer metastatic cells identifies key proteins in cell adhesion, migration, and invasion

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