1. α-Catulin, a Rho signalling component, can regulate NF-κB through binding to IKK-β, and confers resistance to apoptosis
- Author
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Bernd R. Binder, J. van Hengel, Christoph Wiesner, R. de Martin, Martina Hoeth, Johannes A. Schmid, Ulrike Resch, Gabriele Winsauer, and F. Van Roy
- Subjects
Cancer Research ,Apoptosis ,IκB kinase ,Plasma protein binding ,Biology ,Transfection ,Culture Media, Serum-Free ,Growth factor receptor ,Cell Movement ,Serum response factor ,Genetics ,Humans ,Tissue Distribution ,Molecular Biology ,Transcription factor ,Cells, Cultured ,Tumor Necrosis Factor-alpha ,NF-kappa B ,Rho Factor ,I-kappa B Kinase ,Cell biology ,Cytoprotection ,Ectopic expression ,Guanine nucleotide exchange factor ,Inflammation Mediators ,alpha Catenin ,Cytokinesis ,HeLa Cells ,Protein Binding ,Signal Transduction - Abstract
Rho GTPases regulate diverse cellular functions including adhesion, cytokinesis and motility, as well as the activity of the transcription factors NF-kappaB, serum response factor and C/EBP. alpha-Catulin, an alpha-catenin-related protein that shares structural similarities with cytoskeletal linker proteins, facilitates Rho signalling by serving as a scaffold for the Rho-specific guanine nucleotide exchange factor Lbc. We report here that alpha-catulin also interacts with a key component of the NF-kappaB signalling pathway, namely the IkappaB kinase (IKK)-beta. In co-immunoprecipitations, alpha-catulin can bind IKK-beta and Lbc. Ectopic expression of alpha-catulin augmented NF-kappaB activity, promoted cell migration and increased resistance to apoptosis, whereas knockdown experiments showed the opposite effects. Together, these features suggest that alpha-catulin has tumorigenic potential.
- Published
- 2007
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