Signaling through JAM-1 and αvβ3 is required for the angiogenic action of bFGF: dissociation of the JAM-1 and αvβ3 complex

Naik, Meghna U.; Mousa, Shaker A.; Parkos, Charles A.; Naik, Ulhas P.

doi:10.1182/blood-2003-04-1114

Cited by 129 publications

(125 citation statements)

References 39 publications

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“…65e67 An interesting feature of this family of proteins are the tissue-specific functions that seem to be governed by protein distribution patterns and may account for the wide variety of observed functions attributed to various JAMs. A few of the reported functions include regulation of epithelial barrier, 68,69 endothelial and epithelial cell migration, 70,71 spermatogenesis, 72 angiogenesis, 73 and leukocyte adhesion. 74 In addition, JAMs have been linked to roles in the pathophysiology of several disease processes, such as atherosclerosis, 75,76 cancer metastasis, 77 and IBD.…”

Section: Neutrophils Engage Basolateral Epithelial Receptors During Tmentioning

confidence: 99%

Neutrophil-Epithelial Interactions

Parkos

2016

The American Journal of Pathology

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Section: Neutrophils Engage Basolateral Epithelial Receptors During Tmentioning

confidence: 99%

Neutrophil-Epithelial Interactions

Parkos

2016

The American Journal of Pathology

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“…It has been reported previously that JAM-A regulates epithelial and endothelial cell migration (Naik et al, 2003a;Bazzoni et al, 2005;Severson et al, 2008). To confirm that JAM-A regulates cell migration in SKCO-15 cells, we evaluated the effect of decreased JAM-A protein levels on wound closure in a scratch wound assay.…”

Section: Jam-a Regulates Epithelial Cell Migration Through Afadin Butmentioning

confidence: 99%

“…In these cells, JAM-A has been reported to play a role in the regulation of epithelial barrier function (Mandell et al, 2005;Laukoetter et al, 2007), endothelial cell migration (Naik et al, 2003a;Bazzoni et al, 2005), angiogenesis (Naik et al, 2003a), platelet aggregation (Babinska et al, 2002), and leukocyte adhesion (Martin-Padura et al, 1998;Del Maschio et al, 1999). Recent reports suggest that JAM-A not only directly decreases paracellular permeability (Mandell et al, 2005;Laukoetter et al, 2007) but also promotes epithelial cell migration (Severson et al, 2008), which is critical for the maintenance of intestinal barrier in health and disease (Lacy, 1988;Fenteany et al, 2000).…”

Section: Introductionmentioning

confidence: 99%

Junctional Adhesion Molecule A Interacts with Afadin and PDZ-GEF2 to Activate Rap1A, Regulate β1 Integrin Levels, and Enhance Cell Migration

Severson

Lee

Capaldo

et al. 2009

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Junctional adhesion molecule-A (JAM-A) is a transmembrane tight junction protein that has been shown to regulate barrier function and cell migration through incompletely understood mechanisms. We have previously demonstrated that JAM-A regulates cell migration by dimerization of the membrane-distal immunoglobulin-like loop and a C-terminal postsynaptic density 95/disc-large/zona occludens (PDZ) binding motif. Disruption of dimerization resulted in decreased epithelial cell migration secondary to diminished levels of ␤1 integrin and active Rap1. Here, we report that JAM-A is physically and functionally associated with the PDZ domain-containing molecules Afadin and PDZ-guanine nucleotide exchange factor (GEF) 2, but not zonula occludens (ZO)-1, in epithelial cells, and these interactions mediate outside-in signaling events. Both Afadin and PDZ-GEF2 colocalized and coimmunoprecipitated with JAM-A. Furthermore, association of PDZ-GEF2 with Afadin was dependent on the expression of JAM-A. Loss of JAM-A, Afadin, or PDZ-GEF2, but not ZO-1 or PDZ-GEF1, similarly decreased cellular levels of activated Rap1, ␤1 integrin protein, and epithelial cell migration. The functional effects observed were secondary to decreased levels of Rap1A because knockdown of Rap1A, but not Rap1B, resulted in decreased ␤1 integrin levels and reduced cell migration. These findings suggest that JAM-A dimerization facilitates formation of a complex with Afadin and PDZ-GEF2 that activates Rap1A, which regulates ␤1 integrin levels and cell migration.

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“…We also hypothesize that endothelial P2Y 2 R relocation to adherens junctions assists in the transient disruption of endothelial junctions and escorts leukocytes to endothelial borders for paracellular diapedesis, possibly through association of the P2Y 2 R with the α V β 3 integrin. This integrin is known to form a complex with the P2Y 2 R [23] and with JAM-1 [276], a junctional adhesion molecule in endothelial cells that interacts with the leukocyte integrin, LFA-1, and is important for both leukocyte adhesion and diapedesis [277] activation [73]; and the upregulation of tissue factor, an initiator of platelet aggregation [260]. Recently, we found that activation of the P2Y 2 R in human coronary artery endothelial cells causes a rapid translocation of the receptor to cell-cell junctional zones where it interacts with VEcadherin (unpublished results), a protein found specifically in endothelial adherens junctions that is important for maintaining the vascular permeability barrier.…”

Section: Proinflammatory P2y 2 R Functions In Endotheliummentioning

confidence: 99%