A p130 Cas tyrosine phosphorylated substrate domain decoy disrupts v-Crk signaling |
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| Authors: | Kathrin H Kirsch Margaret Kensinger Hidesaburo Hanafusa Avery August |
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| Affiliation: | (1) Immunology Research Laboratories, Department of Veterinary Science, Penn State University, 115 Henning Building, University Park, PA 16802, USA;(2) Laboratory of Molecular Oncology, The Rockefeller University, NY, NY 10021, USA;(3) Department of Biochemistry, Boston University School of Medicine, 715 Albany Street, K-225 Boston, MA 02118, USA;(4) Osaka Bioscience Institute, 6-2-4 Furuedai, Suita Osaka, 565-0874, Japan |
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| Abstract: | Background The adaptor protein p130 Cas (Cas) has been shown to be involved in different cellular processes including cell adhesion, migration and transformation. This protein has a substrate domain with up to 15 tyrosines that are potential kinase substrates, able to serve as docking sites for proteins with SH2 or PTB domains. Cas interacts with focal adhesion plaques and is phosphorylated by the tyrosine kinases FAK and Src. A number of effector molecules have been shown to interact with Cas and play a role in its function, including c-crk and v-crk, two adaptor proteins involved in intracellular signaling. Cas function is dependent on tyrosine phosphorylation of its substrate domain, suggesting that tyrosine phosphorylation of Cas in part regulates its control of adhesion and migration. To determine whether the substrate domain alone when tyrosine phosphorylated could signal, we have constructed a chimeric Cas molecule that is phosphorylated independently of upstream signals. |
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