EGF Receptor Signaling Stimulates SRC Kinase Phosphorylation of Clathrin, Influencing Clathrin Redistribution and EGF Uptake

Wilde, Andrew; Beattie, Eric C.; Lem, Lawrence; Riethof, David A.; Liu, Shuhui; Mobley, William C.; Soriano, Philippe; Brodsky, Frances M.

doi:10.1016/s0092-8674(00)80578-4

Cited by 322 publications

(320 citation statements)

References 46 publications

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“…4B,C). It is known that activated EGFR undergoes endocytosis involving dynamin-regulated and clathrincoated endosomes (Vieira et al 1996;Carter & Sorkin 1998;Wilde et al 1999). Thus, we conclude that the cytoplasmic vesicle structures containing both GFP-P52 and EGFR are endosomes.…”

Section: Egfr Co-localizes With Gfp-shc In Egfstimulated A431 Cellssupporting

confidence: 49%

Adaptor protein Shc undergoes translocation and mediates up‐regulation of the tyrosine kinase c‐Src in EGF‐stimulated A431 cells

Sato

Kimoto²,

Kakumoto³

et al. 2000

Genes to Cells

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Section: Egfr Co-localizes With Gfp-shc In Egfstimulated A431 Cellssupporting

confidence: 49%

Adaptor protein Shc undergoes translocation and mediates up‐regulation of the tyrosine kinase c‐Src in EGF‐stimulated A431 cells

Sato

Kimoto²,

Kakumoto³

et al. 2000

Genes to Cells

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“…The clathrin-dependent pathway has been shown to be the primary pathway for ligand-induced BCR endocytosis, and raft structures appear to be required for efficient phosphorylation of clathrin heavy chain [21,33]. Tyrosine-phosphorylation of clathrin heavy chain is induced by an SRC-type protein kinase in response to stimulation of various receptor types, and the level of phosphorylation correlates with the rate of receptor internalization [21,[34][35][36][37]. Our data support a requirement for phosphorylation of clathrin heavy chain as well as for that of other endocytosis-related factors in BCR internalization.…”

Section: Discussionmentioning

confidence: 99%

Large‐scale proteomic analysis of tyrosine‐phosphorylation induced by T‐cell receptor or B‐cell receptor activation reveals new signaling pathways

et al. 2009

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Activation of the T-cell receptor (TCR) and that of the B-cell receptor (BCR) elicits tyrosinephosphorylation of proteins that belongs to similar functional categories, but result in distinct cellular responses. Large-scale analyses providing an overview of the signaling pathways downstream of TCR or BCR have not been described, so it has been unclear what components of these pathways are shared and which are specific. We have now performed a systematic analysis and provide a comprehensive list of tyrosine-phosphorylated proteins (PY proteome) with quantitative data on their abundance in T cell, B cell, and nonlymphoid cell lines. Our results led to the identification of novel tyrosine-phosphorylated proteins and signaling pathways not previously implicated in immunoreceptor signal transduction, such as clathrin, zonula occludens 2, eukaryotic translation initiation factor 3, and RhoH, suggesting that TCR or BCR signaling may be linked to downstream processes such as endocytosis, cell adhesion, and translation. Thus comparative and quantitative studies of tyrosine-phosphorylation have the potential to expand knowledge of signaling networks and to promote understanding of signal transduction at the system level.

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“…It is known that c-Src mediates internalization of membrane proteins by phosphorylating the internalized protein or components of the internalization machinery [20][21][22]24]. Our results suggest that in this case c-Src may phosphorylate components of the internalization machinery because no tyrosine residue was found in the cytosolic tail of BACE [16,21,23,24,62,63]. Although the precise mechanism of enhanced BACE internalization mediated by c-Src still remains unclear, the results from this study indicate that c-Src may serve as a potential therapeutic target for AD.…”

Section: Discussionmentioning

confidence: 99%

“…Upon activation, RTKs undergo phosporylation at specific tyrosine sites and then bind with SH2 (Src homology region) or PTB (phosphotyrosine binding) domain-containing proteins to activate downstream effectors such as c-Src, MAPK, and PKC [19]. Particularly, c-Src has been demonstrated to regulate the internalization of membrane proteins via different mechanisms [20][21][22][23][24], implicating a means for RTK-mediated regulation of other membrane proteins. RTK internalization is required for their normal signaling.…”

Section: Introductionmentioning

confidence: 99%

Receptor tyrosine kinases positively regulate BACE activity and Amyloid-β production through enhancing BACE internalization

et al. 2007

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Amyloid-β (Aβ) peptide, the primary constituent of senile plaques in Alzheimer's disease (AD), is generated by β-secretase-and γ-secretase-mediated sequential proteolysis of the amyloid precursor protein (APP). The aspartic protease, β -site APP cleavage enzyme (BACE), has been identified as the main β-secretase in brain but the regulation of its activity is largely unclear. Here, we demonstrate that both BACE activity and subsequent Aβ production are enhanced after stimulation of receptor tyrosine kinases (RTKs), such as the receptors for epidermal growth factor (EGF) and nerve growth factor (NGF), in cultured cells as well as in mouse hippocampus. Furthermore, stimulation of RTKs also induces BACE internalization into endosomes and Golgi apparatus. This enhancement of BACE activity and Aβ production upon RTK activation could be specifically inhibited by Src family kinase inhibitors and by depletion of endogenous c-Src with RNAi, and could be mimicked by over-expressed c-Src. Moreover, blockage of BACE internalization by a dominant negative form of Rab5 also abolished the enhancement of BACE activity and Aβ production, indicating the requirement of BACE internalization for the enhanced activity. Taken together, our study presents evidence that BACE activity and Aβ production are under the regulation of RTKs and this is achieved via RTK-stimulated BACE internalization, and suggests that an aberration of such regulation might contribute to pathogenic Aβ production.

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EGF Receptor Signaling Stimulates SRC Kinase Phosphorylation of Clathrin, Influencing Clathrin Redistribution and EGF Uptake

Cited by 322 publications

References 46 publications

Adaptor protein Shc undergoes translocation and mediates up‐regulation of the tyrosine kinase c‐Src in EGF‐stimulated A431 cells

Adaptor protein Shc undergoes translocation and mediates up‐regulation of the tyrosine kinase c‐Src in EGF‐stimulated A431 cells

Large‐scale proteomic analysis of tyrosine‐phosphorylation induced by T‐cell receptor or B‐cell receptor activation reveals new signaling pathways

Receptor tyrosine kinases positively regulate BACE activity and Amyloid-β production through enhancing BACE internalization

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