Identification of Nucleolin as a Novel AEG-1-Interacting Protein in Breast Cancer via Interactome Profiling

AEG-1; LC-MS/MS; breast cancer; metastasis; nucleolin; protein-protein interaction.
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Seong-Jae Lee, Kyoung-Min Choi, Geul Bang, Seo-Gyu Park, Eun-Bi Kim, Jin-Woong Choi, Young-Ho Chung, Jinyoung Kim, Seok-Geun Lee, Eunjung Kim, Jae-Young Kim

  • Cancers (Basel)
  • 0
  • 2021 Jun 7;13(11):2842.
  • Human
  • 抗体芯片
  • 免疫/内分泌
  • 免疫/内分泌
  • 乳腺癌
  • ALK/CD246,EphB4,MuSK,Axl,EphB6,PDGF R alpha,DDR1,ErbB2,PDGF R beta,DDR2,ErbB3,c-Ret,Dtk,ErbB4,ROR1,EGF R,FGF R1,ROR2,EphA1,FGF R2 alpha,Ryk,EphA2,FGF R3,SCF R/c-kit,EphA3,FGF R4,Tie-1,EphA4,Flt-3/Flk-2,Tie-2,EphA5,HGF R/c-MET,TrkA,EphA6,IGF-I R,TrkB,EphA7,Insulin R/CD220,TrkC,EphA10,M-CSF R,VEGF R1/Flt-1,EphB1,Mer,VEGF R2/KDR,EphB2,MSP R/Ron,VEGF R3/Flt-4,EphB3

相关货号

LXAH049-1

Abstract

Breast cancer is one of the most common malignant diseases worldwide. Astrocyte elevated gene-1 (AEG-1) is upregulated in breast cancer and regulates breast cancer cell proliferation and invasion. However, the molecular mechanisms by which AEG-1 promotes breast cancer have yet to be fully elucidated. In order to delineate the function of AEG-1 in breast cancer development, we mapped the AEG-1 interactome via affinity purification followed by LC-MS/MS. We identified nucleolin (NCL) as a novel AEG-1 interacting protein, and co-immunoprecipitation experiments validated the interaction between AEG-1 and NCL in breast cancer cells. The silencing of NCL markedly reduced not only migration/invasion, but also the proliferation induced by the ectopic expression of AEG-1. Further, we found that the ectopic expression of AEG-1 induced the tyrosine phosphorylation of c-Met, and NCL knockdown markedly reduced this AEG-1 mediated phosphorylation. Taken together, our report identifies NCL as a novel mediator of the oncogenic function of AEG-1, and suggests that c-Met could be associated with the oncogenic function of the AEG-1-NCL complex in the context of breast cancer.Keywords:AEG-1; LC-MS/MS; breast cancer; metastasis; nucleolin; protein-protein interaction.
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