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Analysis of protein-protein interactions in cross-talk pathways reveals CRKL protein as a novel prognostic marker in hepatocellular carcinoma.


ABSTRACT: Deciphering the network of signaling pathways in cancer via protein-protein interactions (PPIs) at the cellular level is a promising approach but remains incomplete. We used an in situ proximity ligation assay to identify and quantify 67 endogenous PPIs among 21 interlinked pathways in two hepatocellular carcinoma (HCC) cells, Huh7 (minimally migratory cells) and Mahlavu (highly migratory cells). We then applied a differential network biology analysis and determined that the novel interaction, CRKL-FLT1, has a high centrality ranking, and the expression of this interaction is strongly correlated with the migratory ability of HCC and other cancer cell lines. Knockdown of CRKL and FLT1 in HCC cells leads to a decrease in cell migration via ERK signaling and the epithelial-mesenchymal transition process. Our immunohistochemical analysis shows high expression levels of the CRKL and CRKL-FLT1 pair that strongly correlate with reduced disease-free and overall survival in HCC patient samples, and a multivariate analysis further established CRKL and the CRKL-FLT1 as novel prognosis markers. This study demonstrated that functional exploration of a disease network with interlinked pathways via PPIs can be used to discover novel biomarkers.

SUBMITTER: Liu CH 

PROVIDER: S-EPMC3650343 | biostudies-literature | 2013 May

REPOSITORIES: biostudies-literature

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Analysis of protein-protein interactions in cross-talk pathways reveals CRKL protein as a novel prognostic marker in hepatocellular carcinoma.

Liu Chia-Hung CH   Chen Tzu-Chi TC   Chau Gar-Yang GY   Jan Yi-Hua YH   Chen Chun-Houh CH   Hsu Chun-Nan CN   Lin Kuan-Ting KT   Juang Yue-Li YL   Lu Pei-Jung PJ   Cheng Hui-Chuan HC   Chen Ming-Huang MH   Chang Chia-Fen CF   Ting Yu-Shan YS   Kao Cheng-Yan CY   Hsiao Michael M   Huang Chi-Ying F CY  

Molecular & cellular proteomics : MCP 20130208 5


Deciphering the network of signaling pathways in cancer via protein-protein interactions (PPIs) at the cellular level is a promising approach but remains incomplete. We used an in situ proximity ligation assay to identify and quantify 67 endogenous PPIs among 21 interlinked pathways in two hepatocellular carcinoma (HCC) cells, Huh7 (minimally migratory cells) and Mahlavu (highly migratory cells). We then applied a differential network biology analysis and determined that the novel interaction, C  ...[more]

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