Cell adhesion to fibrillin-1: identification of an Arg-Gly-Asp-dependent synergy region and a heparin-binding site that regulates focal adhesion formation

Bax, Daniel V.; Mahalingam, Yashithra; Cain, Stuart A.; Mellody, Kieran T.; Freeman, Lyle J.; Younger, Kerri; Shuttleworth, C. Adrian; Humphries, Martin J.; Couchman, John R.; Kielty, Cay M.

doi:10.1242/jcs.003954

Cited by 80 publications

(104 citation statements)

References 29 publications

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“…These assemblies were reminiscent of cell-surface LTBP-1 in an earlier scanning-EM study (Taipale et al, 1996). Although both fibrillin-1 and LTBP-1 partially colocalized with fibronectin, exogenous heparin blocked deposition of both LTBP-1 and microfibrils, but not fibronectin; this deposition was most probably blocked by heparin directly competing with heparan-sulfate-dependent fibrillin-1 terminal assembly interactions (Cain et al, 2008) and interactions with syndecans (Bax et al, 2007). Exogenous heparin might also compete with other matrix interactions that depend on cell-surface heparan sulphate.…”

Section: Discussionmentioning

confidence: 74%

“…We have shown that unprocessed N-terminal fibrillin-1 fragment PF1 interacts with cells in a heparan-sulfate-dependent manner (Bax et al, 2007), whereas heparin induces a very high heparin- Ex1-11 and PF1 showed only weak binding to full-length LTBP-1 (not shown). (B)BIAcore analysis of the binding of C-terminal LTBP-1 (C-LTBP-1), immobilized on a CM5 chip, to PF1 (i), PF1 (ii) or PF1 Ex6+7 (iii).…”

Section: Binding Of Full-length Ltbp-1 To Pro-fibrillin-1 Is Facilitamentioning

confidence: 89%

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Assembly of fibrillin microfibrils governs extracellular deposition of latent TGFβ

Massam-Wu

Chiu

Choudhury

et al. 2010

Journal of Cell Science

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142

132

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SummaryControl of the bioavailability of the growth factor TGF is essential for tissue formation and homeostasis, yet precisely how latent TGF is incorporated into the extracellular matrix is unknown. Here, we show that deposition of a large latent TGF complex (LLC), which contains latent TGF-binding protein 1 (LTBP-1), is directly dependent on the pericellular assembly of fibrillin microfibrils, which interact with fibronectin during higher-order fibrillogenesis. LTBP-1 formed pericellular arrays that colocalized with microfibrils, whereas fibrillin knockdown inhibited fibrillar LTBP-1 and/or LLC deposition. Blocking 51 integrin or supplementing cultures with heparin, which both inhibited microfibril assembly, disrupted LTBP-1 deposition and enhanced Smad2 phosphorylation. Full-length LTBP-1 bound only weakly to N-terminal pro-fibrillin-1, but this association was strongly enhanced by heparin. The microfibrilassociated glycoprotein MAGP-1 (MFAP-2) inhibited LTBP-1 binding to fibrillin-1 and stimulated Smad2 phosphorylation. By contrast, fibulin-4, which interacted strongly with full-length LTBP-1, did not induce Smad2 phosphorylation. Thus, LTBP-1 and/or LLC deposition is dependent on pericellular microfibril assembly and is governed by complex interactions between LTBP-1, heparan sulfate, fibrillin-1 and microfibril-associated molecules. In this way, microfibrils control TGF bioavailability.

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Section: Discussionmentioning

confidence: 74%

Section: Binding Of Full-length Ltbp-1 To Pro-fibrillin-1 Is Facilitamentioning

confidence: 89%

Assembly of fibrillin microfibrils governs extracellular deposition of latent TGFβ

Massam-Wu

Chiu

Choudhury

et al. 2010

Journal of Cell Science

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142

132

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“…To evaluate how adhesion to ECM regulates PDGFR activation in MSCs, tyrosine phosphorylation of PDGFR-a and PDGFR-b was examined in serum-free conditions, after plating onto fibronectin, laminin, fibrillin-1 PF8 [an Arg-Gly-Asp (RGD)-containing fragment that engages the a5b1-integrin] (Bax et al, 2007;Cain et al, 2005), collagen type I or collagen type IV (all at 10 g/ml) for 90 minutes. A human array for phosphorylated RTKs (Fig.…”

Section: Adhesion To Ecm Induces Pdgfr Tyrosine Phosphorylationmentioning

confidence: 99%

Mesenchymal stem cell migration is regulated by fibronectin through α5β1-integrin-mediated activation of PDGFR-β and potentiation of growth factor signals

Veevers

Ball

Shuttleworth

et al. 2011

Journal of Cell Science

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203

169

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SummaryCell migration during vascular remodelling is regulated by crosstalk between growth factor receptors and integrin receptors, which together coordinate cytoskeletal and motogenic changes. Here, we report extracellular matrix (ECM)-directed crosstalk between platelet-derived growth factor receptor (PDGFR)-b and a5b1-integrin, which controls the migration of mesenchymal stem (stromal) cells (MSCs). Cell adhesion to fibronectin induced a5b1-integrin-dependent phosphorylation of PDGFR-b in the absence of growth factor stimulation. Phosphorylated PDGFR-b co-immunoprecipitated with a5-integrin and colocalised with a5b1-integrin in the transient tidemarks of focal adhesions. Adhesion to fibronectin also strongly potentiated PDGF-BB-induced PDGFR-b phosphorylation and focal adhesion kinase (FAK) activity, in an a5b1-integrin-dependent manner. PDGFR-b-induced phosphoinositide 3-kinase (PI3K) and Akt activity, actin reorganisation and cell migration were all regulated by fibronectin and a5b1-integrin. This synergistic relationship between a5b1-integrin and PDGFR-b is a fundamental determinant of cell migration. Thus, fibronectin-rich matrices can prime PDGFR-b to recruit mesenchymal cells at sites of vascular remodelling.

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“…Fibrillin can often be found by itself, in which it may independently function as a mechanical, load-bearing but highly extensible scaffold [40]. Numerous domains in fibrillin exist for binding integrins, heparan sulafate proteoglycans, and growth factors, which point to substantial roles for alone fibrillin and mature elastic fibers in mediating cell signaling and adhesion [41].…”

Section: Elastic Fibers Comprise a Significant Portion Of The Ventricmentioning

confidence: 99%

Extracellular Matrix Organization, Structure, and Function

Wiltz¹,

Arevalos²,

Balaoing³

et al. 2013

Calcific Aortic Valve Disease

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Cell adhesion to fibrillin-1: identification of an Arg-Gly-Asp-dependent synergy region and a heparin-binding site that regulates focal adhesion formation

Cited by 80 publications

References 29 publications

Assembly of fibrillin microfibrils governs extracellular deposition of latent TGFβ

Assembly of fibrillin microfibrils governs extracellular deposition of latent TGFβ

Mesenchymal stem cell migration is regulated by fibronectin through α5β1-integrin-mediated activation of PDGFR-β and potentiation of growth factor signals

Extracellular Matrix Organization, Structure, and Function

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