2003
DOI: 10.1074/jbc.m212396200
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Targeting Membrane-localized Focal Adhesion Kinase to Focal Adhesions

Abstract: In the present study, we examined regulation of activated focal adhesion kinase localization in focal adhesions. By using focal adhesion kinase fused to an inert transmembrane anchor, we found that the focal contact targeting region within focal adhesion kinase was preserved in the membrane-targeted fusion protein. However, upon tyrosine phosphorylation, full-length focal adhesion kinase became excluded from focal adhesions. This negative regulation of localization could be abolished by mutating key amino acid… Show more

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Cited by 83 publications
(78 citation statements)
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“…These findings seem to indicate that FAK Tyr 407 phosphorylation might inhibit the access of additional phosphates on Tyr 397 , perhaps because of increased negative charge repulsion. It has been known that FAK molecules phosphorylated at Tyr 397 reside close to the plasma membrane (21,22), and the absence of Tyr 397 phosphorylation decreases its residency at focal adhesions but not in cytosol (22). Consistent with this notion, higher levels of Tyr 407 phosphorylation were observed in cytosolic FAK versus membrane-bound FAK (Fig.…”
Section: Fak Tyrsupporting
confidence: 77%
“…These findings seem to indicate that FAK Tyr 407 phosphorylation might inhibit the access of additional phosphates on Tyr 397 , perhaps because of increased negative charge repulsion. It has been known that FAK molecules phosphorylated at Tyr 397 reside close to the plasma membrane (21,22), and the absence of Tyr 397 phosphorylation decreases its residency at focal adhesions but not in cytosol (22). Consistent with this notion, higher levels of Tyr 407 phosphorylation were observed in cytosolic FAK versus membrane-bound FAK (Fig.…”
Section: Fak Tyrsupporting
confidence: 77%
“…In contrast, CHO cells expressing Y925F FAK mutant were found to migrate at a similar rate to wild-type FAK (Cary et al, 1998). Phosphorylation of this residue may also regulate the localization of FAK to focal adhesions (Katz et al, 2003).…”
Section: Srcmentioning
confidence: 85%
“…While tyrosine phosphorylation of GIT1 residues within the FAH domain does not appear to be an important contributor to binding, as it is in FAK [33], tyrosine phosphorylation elsewhere in GIT proteins does appear important. First, we identified increased binding of paxillin to the Y563F mutant ( Figure 7).…”
Section: Discussionmentioning
confidence: 99%
“…Focal adhesion kinase binding to paxillin through its four-helix bundle FAT domain, and therefore localization to focal adhesions, is regulated in part through phosphorylation of FAK on tyrosine 925, a residue in helix 1 of the FAT domain itself [33]. When phosphorylated at tyrosine 925 by Src family members, FAK is released from focal complexes [33]. We sought to determine whether GIT1 association with paxillin might also be regulated through tyrosine phosphorylation.…”
Section: Nih-pa Author Manuscriptmentioning
confidence: 99%
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