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Differential Protein Expression Profiling by iTRAQ-Two-dimensional LC-MS/MS of Human Bladder Cancer EJ138 Cells Transfected with the Metastasis Suppressor KiSS-1 Gene

机译：iTRAQ二维LC-MS / MS对转移抑制因子KiSS-1基因转染的人膀胱癌EJ138细胞进行差异蛋白表达谱分析

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KiSS-1 is a metastasis suppressor gene reported to be involved in the progression of several solid neoplasias. The loss of KiSS-1 gene expression has been shown to be inversely correlated with increasing tumor stage, distant metastases, and poor overall survival in bladder tumors. To identify the molecular pathways associated with the metastasis suppressor role of KiSS-1 in bladder cancer, we carried out a proteomics analysis of bladder cancer cells (EJ138) transiently transfected with a vector encompassing the full-length KiSS-1 gene using an iTRAQ (isobaric tags for relative and absolute quantitation) approach. Protein extracts collected after 24- and 48-h transfection were fractionated and cleaved with trypsin, and the resulting peptides were labeled with iTRAQ reagents. The labeled peptides were separated by strong cation exchange and reversed phase LC and analyzed by MALDI-TOF/TOF MS. Three software packages were utilized for data analysis: ProteinPilot for identification and quantification of differentially expressed proteins, Protein Center for gene ontology analysis, and Ingenuity Pathways Analysis to provide insight into biological networks. Comparative analysis among transfected, mock, and empty vector-exposed cells identified 1529 proteins with high confidence (>99%) showing high correlation rates among replicates (70%). The involvement of the identified proteins in biological networks served to characterize molecular pathways associated with KiSS-1 expression and to select critical candidates for verification analyses by Western blot using independent transfected replicates. As part of complementary clinical validation strategies, immunohistochemical analyses of proteins regulated by KiSS-1, such as Filamin A, were performed on bladder tumors spotted onto tissue microarrays (n = 280). In summary, our study not only served to uncover molecular mechanisms associated with the metastasis suppressor role of KiSS-1 in bladder cancer but also to reveal the biomarker role of Filamin A in bladder cancer progression and clinical outcome.

机译：KiSS-1是一种转移抑制基因，据报道与几种实体瘤形成有关。已经显示，KiSS-1基因表达的丧失与膀胱癌中肿瘤分期的增加，远处转移和较差的总体生存率呈负相关。为了确定与KiSS-1在膀胱癌中的转移抑制作用有关的分子途径，我们使用iTRAQ（i）进行了用包含全长KiSS-1基因的载体瞬时转染的膀胱癌细胞（EJ138）的蛋白质组学分析（等压标签用于相对和绝对定量）方法。将在24和48小时转染后收集的蛋白质提取物分级分离，并用胰蛋白酶切割，然后将所得肽用iTRAQ试剂标记。通过强阳离子交换和反相LC分离标记的肽，并通过MALDI-TOF / TOF MS分析。三个软件包用于数据分析：ProteinPilot用于鉴定和定量差异表达的蛋白质； Protein Center用于基因本体分析； Ingenuity Pathways Analysis提供对生物网络的洞察力。对转染的，模拟的和空的载体暴露细胞进行比较分析，鉴定出1529种蛋白质（具有高可信度（> 99％）），这些蛋白质在重复样本中具有较高的相关率（70％）。鉴定出的蛋白质参与生物网络有助于表征与KiSS-1表达相关的分子途径，并选择关键的候选物用于通过Western blot使用独立转染的复制品进行验证分析。作为补充临床验证策略的一部分，对点样到组织微阵列上的膀胱肿瘤（n = 280）进行了由KiSS-1调节的蛋白质（如Filamin A）的免疫组织化学分析。总之，我们的研究不仅揭示了与KiSS-1在膀胱癌中的转移抑制作用有关的分子机制，而且揭示了Filamin A在膀胱癌进展和临床结果中的生物标志物作用。

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期刊名称 Molecular Cellular Proteomics : MCP
作者
Isabel Ruppen; Laura Grau; Esteban Orenes-Piñero; Keith Ashman; Marta Gil; Ferrán Algaba; Joaquin Bellmunt; Marta Sánchez-Carbayo;
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年(卷),期 2010(9),10
年度 2010
页码 2276–2291
总页数 16
原文格式 PDF
正文语种
中图分类生化遗传学;生化药理学;
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专利

1. Differential protein expression profiling by iTRAQ-two-dimensional LC-MS/MS of human bladder cancer EJ138 cells transfected with the metastasis suppressor KiSS-1 gene. [J] . Ruppen I, Grau L, Orenes Pinero E, Molecular & cellular proteomics: MCP . 2010,第10期

机译：iTRAQ二维LC-MS / MS对转移抑制因子KiSS-1基因转染的人膀胱癌EJ138细胞进行差异蛋白表达谱分析。
2. Effects of a KiSS-1 peptide, a metastasis suppressor gene, on the invasive ability of renal cell carcinoma cells through a modulation of a matrix metalloproteinase 2 expression. [J] . Yoshioka K, Ohno Y, Horiguchi Y, Life sciences . 2008,第9a10期

机译：KiSS-1肽（一种转移抑制基因）通过调节基质金属蛋白酶2的表达对肾癌细胞的侵袭能力的影响。
3. Expression profiles of proto-oncogene TWIST1 and tumor metastasis suppressor gene LASS2 in bladder cancer [J] . Yegin Zeynep, Aydin Oguz, Koc Haydar, Cellular and molecular biology . 2018,第11期

机译：膀胱癌中的原癌基因Twist1和肿瘤转移抑制基因Lass2的表达谱
4. An iTRAQ-RPLC-MS/MS approach for protein differential expression profiling of MCF7 breast cancer cells: Towards biomarker discovery [C] . Jenny M. Armenta, Iulia M. Lazar ASMS Conference on Mass Spectrometry and Allied Topics . 2008

机译：MCF7乳腺癌细胞蛋白质差异表达分析的ITRAQ-RPLC-MS / MS方法：迈向生物标志物发现
5. LC-MS/MS based metabolic profiling of breast cancer cells. [D] . Zhuang, Shuyi. 2012

机译：基于LC-MS / MS的乳腺癌细胞代谢谱分析。
6. In-depth LC-MS/MS analysis of the chicken ovarian cancer proteome reveals conserved and novel differentially regulated proteins in humans [O] . Angelito I. Nepomuceno, Huanjie Shao, Kai Jing, -1

机译：鸡卵巢癌蛋白质组的深入LC-MS / MS分析揭示了人类保守和新颖的差异调节蛋白
7. Differential Protein Expression Profiling by iTRAQ-Two-dimensional LC-MS/MS of Human Bladder Cancer EJ138 Cells Transfected with the Metastasis Suppressor KiSS-1 Gene* [O] . Ruppen, Isabel, Grau, Laura, Orenes-Piñero, Esteban, 2010

机译：iTRAQ二维LC-MS / MS对转移抑制因子KiSS-1基因转染的人膀胱癌EJ138细胞进行蛋白质差异表达分析*
8. Potential Tumor Suppressor Protein: Expression and Function in Human Breast Cancer Cells [R] . Callaghan, M. 2001

机译：潜在的肿瘤抑制蛋白：人乳腺癌细胞的表达和功能

Differential Protein Expression Profiling by iTRAQ-Two-dimensional LC-MS/MS of Human Bladder Cancer EJ138 Cells Transfected with the Metastasis Suppressor KiSS-1 Gene

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