TRIP6, a Novel Molecular Partner of the MAGI-1 Scaffolding Molecule, Promotes Invasiveness

Overview

Journal FASEB J

Specialties Biology
Physiology

Date 2008 Nov 20

PMID 19017743

Citations 34

Authors

Eric Chastre

Mahmoud Abdessamad

Alexey Kruglov

Erik Bruyneel

Marc Bracke

Yolande Di Gioia

Mary C Beckerle

Frans van Roy

Larissa Kotelevets

Affiliations

Soon will be listed here.

Abstract

We recently established the critical role of the PTEN/MAGI-1b signalosome in stabilization of cell-cell contacts and suppression of invasiveness. The PTEN tumor suppressor is recruited to E-cadherin junctional complexes through the binding to the second PDZ domain of the MAGI-1b scaffolding molecule, whereas beta-catenin interacts with the fifth PDZ domain. To identify additional effectors of this signalosome, we used yeast 2-hybrid screening. Among the clones identified, we focused on TRIP6, which belongs to the zyxin family of proteins. We demonstrated that TRIP6 interacted directly with MAGI-1b by binding to its fifth PDZ domain. Ectopic expression of TRIP6 induced invasiveness in the epithelial MDCK and MDCKts-src cells in a PI3-kinase- and a NF-kappaB-dependent manner and impaired cell-cell aggregation at least in part by uncoupling adherens junctional complexes from the cytoskeleton. The TRIP6Stop473 mutant, which lacks the PDZ binding motif, was still able to increase NF-kappaB and Akt activities but did not promote invasiveness or interfere with cell-cell aggregation. Intracellular delivery of competing peptides corresponding to TRIP6 or beta-catenin C terminus restored invasive properties in MDCKts-src TRIP6Stop473 cells, highlighting the requirement of PDZ scaffolds in junctional complexes activity. TRIP6 overexpression in colon tumors suggest its critical role in cancer progression.

Citing Articles

High Expression Level of TRIP6 is Correlated with Poor Prognosis in Colorectal Cancer and Promotes Tumor Cell Proliferation and Migration.

Ren H, Su Z, Yang J, Cao J, Zhang Y, Sheng K Biochem Genet. 2024; 63(1):261-280.

PMID: 38430448 DOI: 10.1007/s10528-024-10711-x.

TRIP6 a potential diagnostic marker for colorectal cancer with glycolysis and immune infiltration association.

Liu X, Chen Y, Wan H, Wang Y, Wang Y, Gao Y Sci Rep. 2024; 14(1):4042.

PMID: 38369589 PMC: 10874967. DOI: 10.1038/s41598-024-54670-0.

Interactions of the protein tyrosine phosphatase PTPN3 with viral and cellular partners through its PDZ domain: insights into structural determinants and phosphatase activity.

Genera M, Colcombet-Cazenave B, Croitoru A, Raynal B, Mechaly A, Caillet J Front Mol Biosci. 2023; 10:1192621.

PMID: 37200868 PMC: 10185773. DOI: 10.3389/fmolb.2023.1192621.

Amplicon Contains Cyclic AMP Response Element-Driven Gene in Taxane-Resistant MCF-7 Breast Cancer Sublines.

Daniel P, Balusikova K, Vaclavikova R, Seborova K, Ransdorfova S, Valerianova M Genes (Basel). 2023; 14(2).

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The Role of PTEN in Epithelial-Mesenchymal Transition.

Fedorova O, Parfenyev S, Daks A, Shuvalov O, Barlev N Cancers (Basel). 2022; 14(15).

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