A novel signaling molecule, p130, forms stable complexes in vivo with v-Crk and v-Src in a tyrosine phosphorylation-dependent manner.
Ryuichi Sakai,Akihiro Iwamatsu,Naoto Hirano,Seishi Ogawa,Tomoyuki Tanaka,Hiroyuki Mano,Yoshio Yazaki,H Hirai +7 more
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TL;DR: The p130 (designated Cas for Crk‐associated substrate) is a common cellular target of phosphorylation signal via v‐Crk and v‐Src oncoproteins, and its unique structure indicates the possible role of p130Cas in assembling signals from multiple SH2‐containing molecules.
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Abstract: p47v-crk (v-Crk), a transforming gene product containing Src homology (SH)-2 and -3 domains, induces an elevated level of tyrosine phosphorylation of several cellular proteins. Among these proteins, a 125-135 kDa protein (p130) shows marked phosphorylation at tyrosines and tight association with v-Crk, suggesting a direct signal mediator of v-Crk. Here we report the molecular cloning of rat p130 by immunoaffinity purification. The p130 is a novel SH3-containing signaling molecule with a cluster of multiple putative SH2-binding motifs of v-Crk. Immunochemical analyses revealed that p130 is highly phosphorylated at tyrosines during transformation by p60v-src (v-Src), as well as by v-Crk, forming stable complexes with these oncoproteins. The p130 behaves as an extremely potent substrate of kinase activity included in the complexes and it is a major v-Src-associated substrate of the Src kinase by partial peptidase mapping. Subcellular fractionation demonstrated that the cytoplasmic p130 could move to the membrane upon tyrosine phosphorylation. The p130 (designated Cas for Crk-associated substrate) is a common cellular target of phosphorylation signal via v-Crk and v-Src oncoproteins, and its unique structure indicates the possible role of p130Cas in assembling signals from multiple SH2-containing molecules.
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Citations
Comprehensive Summaries of Uppsala Dissertations from the Faculty of Medicine 1211
Tomas Lorant
- 01 Jan 2002
TL;DR: The data suggest the presence of focal adhesion kinase-dependent and -independent pathways for tyrosine phosphorylation of CAS after integrin β1A-mediated adhesion, and the border between the transmembrane and cytoplasmic domains of several integrin subunits was determined.
10
Focal adhesion targeting of v-Crk is essential for FAK phosphorylation and cell migration in mouse embryo fibroblasts deficient src family kinases or p130CAS.
TL;DR: It is suggested that focal adhesion targeting of v‐Crk is essential in v‐ Crk‐mediated cellular signaling and that v‐crk must form a complex with p130CAS or a p 130CAS substitute to transduce signaling from the extracellular matrix.
10
Phosphorylation of Dok1 by Abl family kinases inhibits CrkI transforming activity.
TL;DR: The results support a model in which Dok1 phosphorylation normally suppresses localized Ras pathway activity in Crk-transformed cells via recruitment and/or activation of RasGAP, and that preventing this negative feedback mechanism by inhibiting Abl family kinases leads to enhanced transformation by Crk.
10
The cholecystokinin system in the rat retina: receptor expression and in vivo activation of tyrosine phosphorylation pathways.
TL;DR: The results provide novel biochemical information to further understand the physiological role of CCK A and B receptors in rat retina and demonstrated that they are functional, stimulating tyrosine phosphorylation pathways.
9
An in vivo system for analysis of stable complex formation between Src and AFAP-110
Anne C. Guappone,Yong Qian,Tracy Weimer,Daniel C. Flynn +3 more
- 01 Mar 1996
TL;DR: An in vivo expression system was utilized that permits co-expression of each protein from the same plasmid construct subsequent to transient transfection of Cos-1 cells, allowing for rapid analysis of the mechanism of stable complex formation.
9
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