Extracellular matrix and cell signalling: the dynamic cooperation of integrin, proteoglycan and growth factor receptor

Soo-Hyun Kim; Jeremy Turnbull; Scott Guimond

doi:10.1530/JOE-10-0377

Made available online as an Accepted Preprint 9 February 2011

Extracellular matrix and cell signalling: the dynamic cooperation of integrin, proteoglycan and growth factor receptor

Division of Biomedical Sciences, St George's Medical School, University of London, Cranmer Terrace, London SW17 0RE, UK
¹Institute of Integrative Biology, Centre for Glycobiology, University of Liverpool, Crown Street, Liverpool L69 7ZB, UK

(Correspondence should be addressed to S-H Kim; Email: skim{at}sgul.ac.uk)

Next Section

Abstract

Extracellular matrices (ECM) are secreted molecules that constitute the cell microenvironment, composed of a dynamic and complex array of glycoproteins, collagens, glycosaminoglycans and proteoglycans. ECM provides the bulk, shape and strength of many tissues in vivo, such as basement membrane, bone and cartilage. In vitro, most animal cells can only grow when they are attached to surfaces through ECM. ECM is also the substrate for cell migration. However, ECM provides much more than just mechanical and structural support, with implications in developmental patterning, stem cell niches and cancer. ECM imparts spatial context for signalling events by various cell surface growth factor receptors and adhesion molecules such as integrins. The external physical properties of ECM may also have a role in the signalling process. ECM molecules can be flexible and extendable, and mechanical tension can expose cryptic sites, which could further interact with growth factors or their receptors. ECM proteins and structures can determine the cell behaviour, polarity, migration, differentiation, proliferation and survival by communicating with the intracellular cytoskeleton and transmission of growth factor signals. Integrins and proteoglycans are the major ECM adhesion receptors which cooperate in signalling events, determining the signalling outcomes, and thus the cell fate. This review focuses on the emerging concept of spatial cell biology of ECM, especially the current understanding of integrins and heparan sulphate proteoglycans as the essential cellular machineries that sense, integrate and respond to the physical and chemical environmental information either by directly connecting with the local adhesion sites or by regulating global cellular processes through growth factor receptor signalling pathways, leading to the integration of both external and internal signals in space and time.

Previous Section Next Section

Extracellular matrix as structural support and binding platform

In order for cells to function, they must be properly supported, having contacts with neighbouring cells and/or the extracellular matrix (ECM). The ECM provides much of the structural support available to parenchymal cells in tissues. In the skin, it provides the dermis and the basement membrane, on which sit the basal cells that give rise to the stratified skin layers. All this provides the tensile strength and flexibility inherent to skin. In other tissues, basement membranes provide anchoring support to epithelial and endothelial cells. The ECM is produced by epithelial cells and stromal cells found within the matrix itself, including fibroblasts, osteoblasts and basal epithelial cells.

The primary proteins present in the ECM and indeed the entire body are the collagens. Collagens are a family of proteins with at least 29 members; though not all are found in the ECM, they share a common structural motif of helical fibrils formed by three protein subunits. There are many types of collagens present in the ECM and basement membrane, including, but not limited to type I, III, IV, V and the glycosaminoglycan-containing type XI (Hulmes 2002). The primary function of the collagens is to act as the structural support and binding partners for other ECM proteins. Along with collagen, elastin is the major structural protein in the ECM (Kielty et al. 2002). Individual tropoelastin protein subunits are crosslinked together to give the mature elastin fibre. Elastin, along with fibrillin, is responsible for the flexibility inherent in many tissues.

The diverse array of ECM proteins not only support the physical structure of the cell but also various biological functions, largely through their ability to bind multiple interacting partners such as other ECM proteins, growth factors, signal receptors and the adhesion molecules, which is mediated by the multiple, specific domains present within each protein. The best example is fibronectin (FN), which, like other ECM proteins, is produced by fibroblasts among other cell types. FN exists as a dimer and can bind to collagens and heparan sulphate proteoglycans (HSPGs) (Ruoslahti 1988), also see later section), thus contributing to the structural framework for many cell surface receptor systems. One of the major functional domains contained in FN is the FN type III (FNIII) domain. FnIII domains contain about 100 amino acids in two, anti-parallel β-sheets, which are also present in collagens, neural cell adhesion molecules (NCAMs) and some cytokine receptors. The FNIII domains contain the amino acid sequence responsible for integrin-binding (RGD motif) and heparin-binding domains, which are further discussed later. Two other domains of FN, the FNI and FNII domains, are smaller than the FNIII domains, with 45–60 amino acids, but they share the basic anti-parallel β-sheet structure stabilised by disulphide bonds. The FN domains are primarily responsible for the binding of FN to collagen, fibrin and other FN molecules and are often present in multiple copies within each protein (for example, there are 15 FNIII domains in FN), allowing for multiple interactions, thus providing a protein-binding platform (Ruoslahti 1988). Another well-known example would be laminins, which are mainly present in the basement membranes and partly responsible for providing the tensile strength of the tissue. Laminin consists of three subunits – α, β and γ – which come together to form a characteristic cross pattern that can bind to other laminins as well as proteoglycans and other ECM proteins (Colognato & Yurchenco 2000). Moreover, vitronectin can bind to and regulate components of the plasminogen activator signal complex, in addition to its cell adhesion duties (Preissner & Seiffert 1998).

HSPGs are proteoglycans found in ECM with multiple heparan sulphate (HS) side chains covalently coupled to the core protein. HSPGs present in the matrix include perlecan, agrin, collagen type XI, syndecans and glypicans. The perlecan, agrin and collagens are actively secreted into the ECM, while the syndecans and glypicans are cleaved from the cell surface by proteases and phospholipases respectively (Brunner et al. 1994, Manon-Jensen et al. 2010). Secreted HSPGs bind to almost all of the structural proteins in the ECM via both protein–protein interactions and HS–protein interactions. The cleaved HSPGs interactions are primarily, but not exclusively, via HS chains.

Features of the physical adhesion surface and cell signalling

Studies using fabricated inert matrix substrates such as polyethylene glycol have suggested that the binding interaction of cell surface receptors to specific adhesion ligands can be purely dependent on the mechanical attributes of the surface (Marastoni et al. 2008), and the matrix stiffness has profound effects on cell fate and behaviour (Discher et al. 2009). For example, mesenchymal stem cells differentiate into specific cell types only when grown on the appropriate physiological stiffness; thus, matrix elasticity can direct stem cell lineage specification (Engler et al. 2006). Matrix stiffness also has effects on cell migration, proliferation and survival (Wells 2008), and focal adhesions can form and grow only if they experience pulling forces through their cytoskeleton. It is known that growth on soft substrates leads to smaller focal adhesions, containing less phosphotyrosine, and reduced cytoskeletal organisation (Pelham & Wang 1997); how changes in focal adhesion size and composition as well as other tension-dependent mechanisms drive the genetic programs responsible for the differential responses is under investigation. Through the recent progress in nanotechnology, it is now possible to engineer specific nanopatterned surfaces, providing new insights into the mechanical properties of ECM (Geiger et al. 2001).

Previous Section Next Section

Integrins, the inside-out and outside-in signalling

Cells respond to the mechanical and biochemical changes in ECM through the crosstalk between integrins and the actin cytoskeleton. Integrins are heterodimeric transmembrane receptors composed of eighteen α subunits and eight β subunits that can be non-covalently assembled into 24 combinations. The integrin dimers bind to an array of different ECM molecules with overlapping binding affinities, as summarised in a review by Alam et al. (2007). Therefore, the specific integrin expression patterns by a cell dictate which ECM substrate the cell can bind (Hemler & Lobb 1995) and the composition of integrin adhesomes determines the downstream signalling events, thus the eventual cell behaviour and fate. Integrins have unique ability to respond to the molecular composition and physical properties of the ECM and integrate both mechanical and chemical signals through direct association with the cytoskeleton, which also determines the selection of specific integrin species to be involved (Fig. 1). Integrin recognises and binds to the Arg-Gly-Asp (RGD) motif, which was first discovered in FN but later found in many other ECM proteins including laminin, tenascin, vitronectin and thrombospondin, to name a few (Ruoslahti 1996). The evolutionarily conserved three residue motifs, Arg-Gly-Asp, efficiently serve as the attachment site for integrin-mediated cell adhesion. Both the α and β subunits of integrins bind to RGD sequences and the specificity of integrin binding to different matrix proteins is determined, in part, by other amino acids surrounding the RGD sequence (Ruoslahti 1996). It has been shown that a sufficiently high density of RGD motif that allows a precise spatial distribution pattern of integrins seems to be required to initiate an optimal cellular response (Chen et al. 1997), and spacing between adhesive ligand molecules in a 10–200 nm range seems to mimic physiological properties at focal adhesions (Jiang et al. 2004). Not surprisingly, the short synthetic peptide containing the RGD sequences has been explored to regulate integrin-mediated cell migration, growth, differentiation and apoptosis, as a new therapeutic agent for thrombosis, osteoporosis and cancer (Ruoslahti 1996).

View larger version:

Download as PowerPoint Slide

Figure 1

Mechanisms proposed for growth factor signalling regulation by integrins. (A) The repertoire of integrins expressed on a particular cell can specify the signal pathway due to the differential binding affinity of ECM ligands for the integrins. The tissue stiffness and matrix composition can initiate specific signalling pathways regulating cell behaviour. Clustering and activation of the integrins/actin complexes strengthen the focal adhesion interaction and initiate the framework for cell signalling through assembly of adhesomes. (B) Integrins, via their cytoplasmic domain, recruit specific adaptors to the plasma membrane, which regulate the growth factor receptor signalling. For example, β1c integrin recruits Gab1/Shp2 and presents Shp2 to IGF1R, resulting in dephosphorylation of the receptor (Goel et al. 2005). (C) In response to growth factor stimulation, integrins co-localise at focal adhesion with the growth factor receptors and their associated signalling molecules, such as Src and FAK, as well as with cytoskeletal molecules such as paxillin, talin, and vinculin. For example, the α2β1 integrin co-localises with EGFR (Yu et al. 2000), which eventually regulate the activity of the downstream effectors such as ERK, AKT, JNK, and the Rho GTPases. The details of these downstream pathways can be found in other recent reviews (Legate et al. 2009). (D) Integrins can change the rate of growth factor receptor internalisation and degradation. One such example is the interaction of EGFR1 and α5β1 integrin, which is co-ordinately recycled to the plasma membrane, regulating the protein kinase B (PKB) signalling (Caswell et al. 2009). Integrin-mediated cell adhesion can also alter PDGFR rate of degradation via ubiquitination (Baron & Schwartz 2000).

Diverse molecular interactions at the adhesion sites

Integrins are the main cell adhesion receptors involved in focal adhesion formation and are required for cell migration. The scaffolding interactions of integrins to the actin cytoskeleton involve actin polymerising and actin linking molecules, whose interactions regulate, and are regulated by, the associated adhesion signalling molecules (Mitra et al. 2005). When inactive, integrins are unable to bind to ECM or other receptors, which is important for circulating cells such as lymphocytes. The initial assembly of the nascent adhesion is mediated by anchoring proteins called talins, whose amino terminus interacts with the cytoplasmic tail of the β integrin subunit, while the carboxyl termini of talins bind actin. However, to achieve maximal integrin activation, the cooperation of another anchoring protein, kindlin, which binds to β integrin tails distinct from those used by talin is required (Moser et al. 2008). The synergistic effect of talin and kindlin on the activation and the assembly of adhesion structures is enhanced by the binding of vinculin to talin, which triggers the clustering of activated integrins/actin complexes, further strengthening the focal adhesion interaction (Galbraith et al. 2002). The progression from the rather unstable nascent adhesions to dot-like focal complexes upon recruitment of vinculin leads to the formation of larger focal adhesion assembly and the conformational transition of the entire α–β integrin dimers to their active state capable of high-affinity interactions with ECM ligands, eventually leading to maturation of fully activated streak-like fibrillar focal adhesions which can transmit the signal (Tadokoro et al. 2003).

The turnover of focal adhesions is essential for cell motility, and the formation of the actin stress fibre usually occurs underneath the lamellipodia at the leading edge of the cell protrusion. Lamellipodia are the thin, flat extensions of plasma membrane formed by a dynamic network of actin polymerisation mediated by the actin-related protein 2/3 (Arp2/3) complex, and generates mechanical forces that alter local cytoskeletal dynamics. These physical cues, in turn, cause changes in cell shape and motility and eventually gene transcription, regulating cell migration and differentiation (Geiger et al. 2001, 2009, Humphries et al. 2007, Choi et al. 2008).

Database mining, combined with an extensive literature search, recently identified a large number of molecules that comprise the ‘integrin adhesome’ (Zaidel-Bar et al. 2007). The integrin adhesome consists of up to 156 distinct components, most of which are a fundamental part of the adhesion sites, while others may only transiently associate with the adhesion site to influence the structures or signalling activity. As the cytoplasmic domains of integrins have no catalytic activity of their own, they must recruit accessory molecules, which contribute to the actin cytoskeletal reorganisation and endow catalytic activity to the focal adhesion. The integrin adhesome-associated proteins include a diverse range of kinases, phosphatases and adaptor proteins, which contribute and initiate cascades of signalling events (Fig. 1). Several tyrosine kinases and phosphatases are shown to be localised to focal adhesions, which are necessary for the regulation of mechano-sensory activity of focal adhesions; these include focal adhesion kinase (FAK), Src, receptor type tyrosine protein phosphatise α (RPTPα) and SH2 domain-containing protein tyrosine phosphatase 2 (SHP2; Tilghman & Parsons 2008).

Src–FAK: the focal point for integrin signalling

One of the earliest signalling events upon the integrin ligation and clustering, thus transducing extracellular cues to the cytoskeleton, is the activation of the tyrosine kinases Src and FAK. FAK is a non-receptor tyrosine kinase which gets activated upon integrin binding to autophosphorylate Y397 – this induces subsequent binding of Src by the SH2 domain, leading to stable and increased activation of Src–FAK complex. Src further phosphorylates FAK and several downstream binding partners (Brown et al. 2005). Src is a non-receptor tyrosine kinase associated with the cytoplasmic tail of β3 integrins via its SH3 domains. The Src kinase family consists of nine members including Src, Fyn and Yes, and the phosphorylation of Src leads to activation of JNK (Arias-Salgado et al. 2003). One of the targets of the FAK is Rho (Hanks et al. 1992). The Rho family of GTPases, including Rac, Cdc42 and RhoA, cycles between an active GTP-bound form and an inactive GDP-bound form and link the actin polymerisation at focal adhesions to the global actin dynamics (Jaffe & Hall 2005). FAK activation also leads to the recruitment of PI3 kinase to focal adhesion, leading to activation of AKT, a ubiquitously expressed serine/threonine kinase that regulates integrin-mediated cell survival. Moreover, FAK represents a crosstalk point for growth factor receptor pathway, since the signals from integrins–Src–FAK complex can be integrated with that of growth factors and be transmitted through the same Ras–MEK–MAPK pathway, which modulates both focal adhesion dynamics and cellular functions (Kim & Kim 2008). Although growth factors can activate the Ras pathway independently of adhesion, studies have shown that activation of MEK1 and Raf1 by adhesion-mediated signalling through Src–FAK is necessary for the signal to proceed to MAPK activation. Thus, MEK1 and Raf1 are critical convergence points between growth factor and integrin signalling (Slack-Davis et al. 2003, Edin & Juliano 2005; Fig. 1).

Further insights into how these signalling molecules are assembled within the spaces of the plasma membrane structure have emerged from the studies on lipid rafts. Integrin clustering induces reorganisation of the plasma membrane into a highly ordered specific subclass of lipid rafts – caveolae – around the focal adhesion, which effectively concentrate the multi-protein signalling complex. It has been shown that integrins associate with Src and FAK within caveolae (Park et al. 2011). Furthermore, caveolin-1, the main component of caveolae, gets phosphorylated during focal adhesion signalling in migrating cells and integrin-regulated caveolae trafficking (Salanueva et al. 2007). Any changes in integrin ligand binding can also effectively turn off the entire signalling modules by rapid internalisation at the caveolae (del Pozo et al. 2004). Growth factor receptors often localise to caveolae and are known to be regulated by receptor trafficking and internalisation. Further investigation on how the assembly of integrin complexes, the plasma membrane order and the processes of endocytosis are coordinated in a three-dimensional environment, thus providing the spatial regulation of signal transduction pathways, is awaited (Fig. 1).

Previous Section Next Section

ECM as the organising centre for growth factor receptor signal regulation

ECM proteins play crucial and complex roles during cell surface receptor signalling. First of all, ECM serves as a reservoir for growth factors. ECM-bound growth factors could be released locally and bind to their canonical receptors. Many ECM proteins have binding sites for both cell adhesion and growth factors, allowing local concentration of the growth factors near to their cell surface receptors and cell adhesion sites. This localisation of growth factors, and thus their signalling, by the ECM probably contributes to the establishment of gradients of the soluble, diffusible growth factor morphogens, which play vital roles in patterning in developmental processes (Kirkpatrick et al. 2004, Kreuger et al. 2004). Such examples include fibroblast growth factors (FGFs) and vascular endothelial growth factors (VEGFs), both of which bind to HSPG and can be cleaved off from the glycosaminoglycan components of HSPG by the enzyme heparanase and released as soluble ligands (Patel et al. 2007), which are discussed in detail later. However, ECM-bound growth factors do not have to be released in soluble form to function. In fact, it is well established that FGFs actually bind to their receptors with HS as a cofactor, with the HSPG ‘presenting’ these ligands during signalling. Other examples are FN and vitronectin, both of which bind to hepatocyte growth factor (HGF) and form complexes with Met (the HGF receptor) and integrins, either positively or negatively regulating the functions of the diffusible morphogen HGF. In this regard, ECM can also function as an organising centre of the signalling complex on the cell surface.

The binding of ECM with growth factors often involves specific domains of ECM proteins and results in modulation of signalling activities. For instance, FnIII domains in both FN and tenascin-C bind to VEGF, which potentiates the VEGF-mediated signalling through its receptor VEGFR2 (Wijelath et al. 2006). FnIII domains of ECM-associated protein anosmin-1 are shown to bind to FGFR1 ectodomains and function as a co-ligand for FGFR1 signal complex, enhancing or inhibiting the activity (Hu et al. 2009). Similarly, Drosophila collagen IV binds to Dpp, a bone morphogenetic protein (BMP) homologue, and enhances interactions with BMP receptors (Wang et al. 2008). Collagen II, the major collagen of cartilage, contains a chordin-like VWC domain, which binds to transforming growth factor β1 (TGF-β1) and BMP-2, acting as a negative regulator for these essential chondrogenic growth factors (Garcia et al. 2002). On the other hand, some intrinsic domains within ECM proteins can act as non-canonical ligands for the receptors. Many ECM proteins including laminin, tenascin, thrombospondin and fibrillin contain epidermal growth factor (EGF)-like domains which can directly bind to EGF receptor as soluble ligands and modulate its signalling (Schenk et al. 2003). FnIII domains of NCAM bind directly to FGFR1 and can induce ligand-independent receptor phosphorylation (Kiselyov et al. 2003). However, further investigation is needed to determine if there is any difference between the ECM-associated growth factor-like ligands (either acting from the anchored solid-phase or as released soluble form) and the canonical ligands in terms of the specific signalling outcome.

Integrin and growth factor receptor signalling

Integrins can activate several signalling pathways independently (Assoian & Schwartz 2001), but more frequently they act synergistically with other growth factor receptors (Alam et al. 2007). Such examples include insulin receptor (Schneller et al. 1997); type 1 insulin-like growth factor receptor (IGF1R; Zhang & Yee 2000); VEGF receptor (Ruoslahti 2002), TGF-β receptor (Scaffidi et al. 2004), HGF receptor (c-Met) (Sridhar & Miranti 2006), platelet-derived growth factor-β (PDGF-β) receptor (Schneller et al. 1997) and EGF receptor (Bill et al. 2004). The functional activities of these growth factor receptors are dynamically and reciprocally controlled by integrins. The fact that growth factor signalling requires the presence of specific integrin subunits and that different cell types express different profiles of integrins may constitute the ‘cellular context’ determining the outcome of the growth factor signal (Alam et al. 2007).

Role of proteoglycans in signal regulation

Traditionally, there were two functions ascribed to HSPGs in the matrix (David 1992, Hardingham & Fosang 1992). The first was to contribute to the organisation of the matrix by binding to the many core matrix molecules via HS chains (e.g. laminin, FN and collagen). The second was to act as an extracellular storage mechanism for heparin-binding growth factors such as FGFs secreted by stromal cells. The HSPGs would control the diffusion of the growth factors to establish protein gradients, such as during development, or act as a repository of growth factors that could be sequestered from cells and released at an appropriate time, such as wound healing (Zcharia et al. 2005). More recently, however, it has been identified that the HS chains play a more proactive role.

The ability of heparin (a highly sulphated form of HS found in connective tissue mast cells and often used as the source of HS in experiments) to bind to many proteins has been known for many years. Heparin can bind to many different classes of proteins, ranging from growth factors (FGFs, VEGFs, PDGF, glial cell-derived neurotrophic factor (GDNF), and HGF) to cytokines (interleukins, interferon, PF4, and RANTES), metabolic enzymes (lipoprotein lipase) and structural proteins (laminin and FN), among many others (Kjellen & Lindahl 1991, Casu & Lindahl 2001). HS-binding domains in these proteins are not usually defined by their structural motifs, but rather typically characterised by a collection of basic residues, such as arginine and lysine, that are in close proximity either in the linear amino acid sequence as found in FGFR or through protein folding as found in FGF-1 (Kan et al. 1993, Wong et al. 1995, Blaber et al. 1996). As such there is no general consensus sequence for identifying HS-binding domains in proteins. In the past, HS-binding sequences have been identified empirically using mutation of lysine and arginine residues, structural studies such as nuclear magnetic resonance (NMR) and X-ray crystallography and by protease protection assays, where the region of the protein bound by heparin is protected from protease digestion and the resulting peptide fragments can be identified by mass spectrometry (Ori et al. 2009).

Most of the protein-binding activity of HSPGs is contributed to the HS chains. The average HS chain is 50–200 repeating disaccharide units in length, which is synthesised by the sequential addition of a xylose, galactose, galactose and d-glucuronic acid motif on a serine residue of the core protein. The next sugar to be added is N-acetyl glucosamine. Following this, two enzymes, EXT1 and EXT2, polymerise the chain with the addition of alternating d-glucuronic acid and N-acetyl glucosamine. There is then a series of sequential modification reactions carried out by families of sulphotransferase enzymes that generate the diversity of HS seen in tissues (Lindahl et al. 1989, Turnbull & Gallagher 1990, Esko & Selleck 2002). It is important to note that these enzyme reactions do not go to completion and that any given cell may express only a subset of the available biosynthetic enzymes, thus generating the structural diversity of HS. Other factors include posttranscriptional and posttranslational regulation of the enzymes (Pinhal et al. 2001, Grobe & Esko 2002, Nagai et al. 2004) and the action of extracellular Sulf enzymes, which remove 6-O sulphates on HS after it has been synthesised (Lamanna et al. 2006).

The sulphate residues and the carboxylic acid group are largely responsible for the ionic interactions between HS and proteins, but hydrogen bonding and van der Waals interactions also make a significant contribution to the binding energy (Faham et al. 1996). However, binding and regulation of proteins by HS is not solely down to the linear sequence of the sulphates present. The conformation of the HS is also suspected to determine its protein-binding properties (Skidmore et al. 2008). There are several ways that a certain conformation can be achieved. The presence or absence of specific sulphate groups and the identity of the uronic acid affect the conformation of the sugar residues and thus the overall conformation of the molecule (Rudd et al. 2008). The conformation can also be affected by the associated cation present with the molecule, which in turn affects the biological activity of HS (Rudd et al. 2008, Guimond et al. 2009).

Perlecan is a major HSPG found in the basement membrane-like structure around chondrocytes, and binds to many growth factors, including FGFs and VEGFs (see below), thus involved in regulating proliferative and migratory signals in response to growth factor signals during differentiation, cancer and angiogenesis. Perlecan is shown to have both pro-angiogenic and anti-angiogenic capacities (Whitelock et al. 2008).

The other major proteoglycan components of the ECM are the chondroitin sulphate proteoglycans (CSPGs). Unlike the HSPGs, there are a large number of CSPG core proteins secreted directly into the matrix, including aggrecan, versican, brevican and the small, leucine-rich proteoglycans such as decorin and biglycan among others (Kresse & Schonherr 2001). Some of the CSPGs can be quite large (MW>10 00 000) and bind to many different components of the ECM, effectively crosslinking them. CSPGs also bind to and regulate a number of growth factors, such as members of the TGF family (Hildebrand et al. 1994).

Hyaluronic acid is a glycosaminoglycan consisting of alternating glucuronic acid and N-acetyl glucosamine sugars. Hyaluronic acid is different from the other glycosaminoglycans in that it is synthesised on the cell surface and not covalently linked to a core protein during synthesis. It is very hydroscopic and is responsible for the gel-like consistency of tissues such as cartilage (Day & Sheehan 2001).

Role of HSPG in FGF and VEGF signalling

The binding specificity of FGFs to FGFRs is partly dictated by the receptor isoform (Ornitz et al. 1996). Notably, these FGF/FGFR binding interactions were all determined in the presence of heparin. HS can influence the FGF binding specificity and activation of FGFR, and indeed particular HS structures can block or inhibit the signalling process. It must be noted that the ability of HS to bind a protein does not necessarily support a positive biological activity; for example, structures have been identified that can bind to FGF-2 but not support its signalling through FGFR1 (Turnbull et al. 1999, Guimond et al. 2006). The potential mechanisms of HS-mediated regulation of FGF signalling are illustrated in Fig. 2. Three different types of HS structures characterised by the presence of different sulphate groups are depicted as three different coloured boxes (red, yellow, or green). Only one of these HS structures (represented by the green box) can allow FGF binding as well as activate the FGFR, while another HS structure (represented by the red box) can bind to FGF, but cannot support its binding to FGFR. PDGF binding to a third type of HS sequence (yellow box) is not affected and may have a different regulatory role in PDGF signalling activity (Fig. 2).

View larger version:

Download as PowerPoint Slide

Figure 2

Different HS structures support different biological activities. (A) Heparan sulphate that has different cell- and tissue-specific structures (denoted schematically by red, yellow and green bars) with binding domains for different growth factors. Here, green represents structures that are capable of binding to both FGF and FGFR, thus supporting ligand-induced dimer formation and consequent signalling in the FGFR complexes. Yellow structures cannot bind to FGF or FGFR, but are capable of binding to PDGF and regulating its activity. Red structures can bind to FGF, but cannot support subsequent binding to FGFR. (B) Heparan sulphate that lacks the required structures (green) cannot support FGF signalling through FGFR, although the presence of other structures (red) still allows it to bind to FGF without supporting its activity. Other structures (yellow) may bind and regulate PDGF, mediating alternative signal pathway.

VEGF is another example of essential growth factor, whose spatially restricted distribution during development is mediated by the binding of HS. The precise deposition and expression of specific isoform of VEGF with a differential binding affinity for HSPG regulate endothelial cell proliferation, migration, differentiation and survival, which is necessary for appropriate pattern formation and tissue morphogenesis in mice (Ruhrberg et al. 2002).

Perlecan co-localises with FGF2 and acts as a mechanotransducer and mitogen for chondrocytes through the activation of MAP kinases (Vincent et al. 2007). Interestingly, perlecan can be substituted not only with HS but also with chondroitin sulphate. Nonetheless, HS chains of perlecan seem to favour FGF/FGFR interaction, while chondroitin sulphate chains in perlecan act as a negative regulator of FGF/FGFR by sequestering the FGFs from their cognate receptors (Whitelock et al. 2008). It has also been shown that different isoforms of VEGFs exhibit differential binding to the HS side chains of perlecan, thus affecting the VEGF signalling outcome as well as creating differential gradient of the ligand at the cell surface (Robinson & Stringer 2001, Whitelock et al. 2008). VEGF has also the ability to displace FGF from the ECM, potentially inducing a synergy between the VEGF and FGF pathways during angiogenesis (Kamei et al. 2010).

Previous Section Next Section

ECM proteases and heparanase

Cell movement and tissue remodelling are important both physiologically (e.g. during development) and pathologically (e.g. wound healing and cancer metastasis). In order for these processes to occur, the ECM must be degraded to allow the free movement of cells or the processing and deposition of new matrix. These processes are accomplished by proteases and also the HS-degrading enzyme heparanase. There are two well-known families of proteases that are involved in the biology of the ECM, the matrix metalloproteinase (MMP) and the A disintegrin and metalloproteinase with thrombospondin motif (ADAMTS) families.

Matrix metalloproteinases

MMPs are a family of 24 proteins in mammals (Yong 2005, Shiomi et al. 2010). Six of these are associated with cell membranes via glycosylphosphatidylinositol anchors (MMP17 and 25) or protein transmembrane domains (MMP14, 15, 16, and 24) and the rest are secreted. Others can be associated with cells via interactions with other proteins, such as MMP9 with CD44 and MMP7 with HSPGs and integrins (Yu et al. 2002). It is the cell-associated MMPs that are responsible for the majority of ECM degradation. MMPs can also cleave other proteins such as growth factors and cell adhesion molecules, in some cases releasing active molecules (Mott & Werb 2004). The activity of the MMPs is highly regulated since inappropriate degradation of matrix would compromise the integrity of tissues (Overall & Lopez-Otin 2002). The first point of regulation is at the level of transcription. Secondly, the MMPs are made as inactive zymogens that require processing before they can degrade matrix. Related to this is the fact that some MMPs, such as MMP14 and tissue inhibitors of metalloproteinase-2 (TIMP-2), must be associated with cell surface proteins prior to activation (Apte et al. 1997). In addition, there are a family of inhibitors of MMPs, including TIMPs that regulate the activity of the active enzyme (Brew & Nagase 2010). Due to their ability to degrade matrix and activate proteins such as growth factors, the MMPs are involved in a number of disease processes, particularly in the CNS, including inflammation, neuronal regeneration and stroke (Yong 2005). The expression of several MMPs, such as MMP 1, 2 and 3, increases in models of multiple sclerosis (Weaver et al. 2005). MMP7 expression also increases during spinal cord injury (Wells et al. 2003).

A disintegrin and metalloproteinase with thrombospondin motif

There are 19 members of the ADAMTS family, which are related to the ADAM transmembrane proteases responsible for processing membrane-bound precursor proteins such as Notch, Delta and HB-EGF (Tang 2001, Shiomi et al. 2010). ADAMTS family shares a common domain structure, including, but not limited to, the Zn²⁺-dependent catalytic domain, a disintegrin domain, a thrombospondin repeat domain and cysteine-rich domains. These proteases bind to both the cell surface and ECM proteins via a spacer domain between the thrombosopondin repeat domains and the C-terminal domain of the protein. Similar to the MMPs, they can be inhibited by the TIMPS and made as inactive zymogens that must be proteolytically cleaved to become active.

While the MMPs are generally broad-spectrum proteases, some of the ADAMTS play specific roles in the processing of the ECM. ADAMTS2 cleaves pro-collagen to collagen to allow fibril formation (Colige et al. 1999); hence, mutations of ADAMTS2 are responsible for a subtype of Ehlers–Danlos syndrome. ADAMTS4 cleaves aggrecan in cartilage (Tortorella et al. 1999), and has a role in the development of osteoarthritis. Other ADAMTS proteins have been implicated in inflammation (Tang 2001).

Heparanase

Besides the degradation of the protein component of the ECM, HS can also be degraded. The enzyme heparanase is an endoglucuronidase that cleaves between the uronic acid and glucosamine of HS (Hulett et al. 1999, Vlodavsky et al. 1999). The cleavage of HS accomplishes three objectives: the removal of a vital crosslinker of matrix proteins, the release of growth factors bound to HS that can subsequently act on cells and the release of oligosaccharides of HS that can regulate protein–protein binding, all of which are crucially important for cell migration and tissue remodelling during development. However, these very same properties can contribute to pathologic conditions such as angiogenesis during wound healing (Dempsey et al. 2000) and inflammation (Li & Vlodavsky 2009), where heparanase has been investigated as a therapeutic target for new treatments.

Previous Section Next Section

Role of ECM in endocrine disease and cancer

Recent studies have revealed the role of ECM in many pathologic conditions; defects in ECM assembly can have a direct or an indirect effect as a consequence of mis-regulated receptor signalling. The progressive changes in ECM composition and organisation in the diseased tissue can induce a variety of genetic and biological alterations, including amplification or inactivation of specific signal pathways, expression of disease markers and aberrant cell and tissue architecture. When epithelial cells are detached from ECM, they undergo cell death, namely anoikis or autophagy, again supporting the notion that cell adhesion to ECM is critical for cell survival and growth (Lock & Debnath 2008, Marastoni et al. 2008).

ECM and the endocrine system

Many aspects of endocrine system development and pathology have interdependent relationships with the ECM. Sertoli cells and testicular peritubular cells cooperate in the synthesis and deposition of ECM components in the formation of the basal lamina of the seminiferous tubule (Skinner et al. 1985). FSH increases the activity and biosynthesis of ECM-associated protease, tissue-type plasminogen activator, during the initial granulosa cell development in the ovary (Knecht 1988). Stress hormones such as norepinephrine and epinephrine can contribute to ovarian cancer progression by activating FAK, which protects the cancer cells from anoikis (Sood et al. 2010). Pancreatic fibrosis, which is characterised by stromal expansion and the excessive deposition of ECM replacing pancreatic tissue, underlies many major endocrine diseases, including pancreatic cancer, chronic pancreatitis and type 2 diabetes mellitus. The detailed molecular mechanisms are still unclear, but recent evidence indicates that ECM-dependent EGFR signalling may regulate pancreatic fibrogenesis in vivo (Blaine et al. 2009). The importance of optimal ECM re-establishment for human pancreatic islet culture has been recently highlighted. The interactions between islet cells and ECM are essential for normal islet physiology; thus, the biggest challenge for the researchers is how to overcome apoptosis (anoikis) caused by the loss of the ECM upon islet cell isolation and subsequent in vitro culture condition. A recent study demonstrated that the various ECM components, including collagen I and IV, FN and laminin can exert different effects on human islet adhesion, survival and functionality (i.e. structural integrity, insulin gene expression and release and glucose metabolism-related gene expression) (Daoud et al. 2010).

ECM also plays key roles in the reproductive function. In most of the mammals, large amount of hyaluronan is synthesised by the cumulus cells before ovulation and organised into ECM, a process called cumulus expansion, which provides an essential microenvironment for oocyte fertilisation. Interestingly, RhoA activation induces resistance of the cumulus to hyaluronidase and sperm penetration, indicating integrin and consequent ECM remodelling through the Rho are required for successful fertilisation (Yodoi et al. 2009).

Renal hypertrophy and abnormal ECM deposition are hallmarks of diabetic nephropathy and it has been proposed that MMP-mediated breakdown and turnover of ECM in the glomerulus underlies the renal pathology (Thrailkill et al. 2009).

ECM as tumour microenvironment

The role of ECM in tumourigenesis has been intensively studied. It has become increasingly clear that cancer does not result from unregulated growth of a single cell, but rather involves multiple dysfunctions of interactions between various cell types and malignant alteration of the tissue microenvironment. The recent identification of cancer stem cells and the epithelial–mesenchymal transitions have brought further support to this concept. Metastatic tumours arise when the cancer cells gain the capacity to degrade the normal tissue architecture and migrate out into interstitial spaces and eventually to different sites after breaking away from the surrounding ECM boundaries (Wiseman & Werb 2002). The microenvironment surrounding the malignant cells is called the tumour stroma, which contains the tumour-derived non-malignant cells, including endothelial cells, pericytes, fibroblasts, tumour-associated macrophages and immune cells (CD4+ and CD8+T lymphocytes, B lymphocytes and Natural Killer cells), with a multitude of growth factors and angiogenic factors like VEGFs embedded in the ECM. Both the stromal and cancer cells produce proteases that continuously remodel the ECM (Kalluri & Zeisberg 2006), and a five-step process of ECM remodelling concomitant to the tumour cell migration has been proposed (Friedl & Wolf 2009). In fact, almost all aspects of cancer formation (e.g. growth, differentiation, motility, and apoptosis) and their signal transduction networks can be regulated by physical interactions between ECM and the cells. For instance, normal function of epithelia is critically dependent on the basement membrane, a highly specialised ECM which contains type IV collagen, laminin, types XV and XVIII collagens, perlecan and nidogen (Kalluri 2003). Progressive loss of an intact basal lamina is the first stage of the neoplastic disorganisation and the breakdown of boundaries during metastatic invasion (Ingber et al. 1981). In a rat model, chemical carcinogens must be applied both on the basement membrane and the epithelium to induce mammary gland cancer, suggesting that alteration of the stroma is essential for carcinogenesis and mutations in the epithelium alone is not sufficient (Maffini et al. 2004). Interestingly, overexpression of the ECM-degrading enzyme MMP3/stromelysin-1 in transgenic mice induces the transformation of normal breast epithelium into cancerous tissue, which exhibits genomic abnormalities; therefore, structural or mechanical changes in the tissue microenvironment may contribute to the genetic reprogramming of the cancer cells (Sternlicht et al. 1999). Conversely, stroma from healthy animals can restore normal characteristics of epithelial cancer cell implants (Maffini et al. 2005), and integrin-blocking antibodies were shown to revert the malignant phenotype of human breast cells (Weaver et al. 1997). This is somewhat controversial, since it has long been believed that cancer is an irreversible disease that results from accumulated gene mutations and chromosomal abnormalities. However, it seems possible for cancer to be induced to become quiescent or revert to a normal state, if provided with the correct set of ECM signals, similarly to the normal embryogenesis (Kenny & Bissell 2003).

Collagen is the major structural component in the formation of solid tumours and collagen fibre density can contribute to tumour initiation, invasion and metastasis (Gao et al. 2010, Kakkad et al. 2010). It has been shown that the increased expression of lysyl oxidase (LOX), an enzyme that covalently crosslinks collagen and elastin, is responsible for excess collagen deposition and hypoxia-induced metastasis of lung cancer through induction of β1 integrin signalling (Gao et al. 2010). Kakkad et al. (2010) also report that hypoxia causes reduction of collagen I fibre density and restructuring of the ECM, thus contributing to the tumour cell dissemination.

A wealth of information has been generated on the integrin family playing a critical role in tumourigenesis and metastasis by modulating the activities of growth factor receptors, extracellular proteases and chemotactic molecules, which can be found in other excellent reviews (White & Muller 2007, Desgrosellier & Cheresh 2010) and such importance of integrins in tumour progression of multiple cell type has made them an attractive anti-cancer target.

HSPG in disease mechanisms

There is a growing body of evidence that HS changes naturally during many physiologic processes. During normal mouse brain development, there are changes in chain length and 6-O sulphation that occur as the neural epithelium develops (Brickman et al. 1998). These changes have functional consequences on the ability of the HS to promote FGF activity (Guimond & Turnbull 1999). Phage display antibodies to HS (van Kuppevelt et al. 1998) with different levels of sulphation or natural HS protein ligands have been used to identify spatial and temporal differences in HS expression during development (Friedl et al. 2001, Allen & Rapraeger 2003). Differences in HS within tissues are not restricted to physiologic processes. Because of the ability of HS to regulate the activities of many growth factors, alterations in HS structure could be a contributing factor in the progression of many tumours. For example, removal of 6-O sulphates can reduce tumour growth in vivo (Narita et al. 2006), and HSPGs from normal versus malignant epithelial cells show differences in their ability to support FGF-2/FGFR complex formation (Mundhenke et al. 2002). Stromal fibroblasts expressing high levels of syndecan-1, a HSPG core protein, enhanced the attachment of breast carcinoma cells and the establishment of cancer microenvironment permissive to the cancer cell migration and invasion (Yang et al. 2011). Basement membranes of renal cell carcinomas show altered ability to bind to members of the FGF family in an HS-dependent manner (Friedl et al. 1997). It is not known whether any or all such changes are a consequence of the progression of a cell from normal to cancerous, but the ability of HS to regulate many proteins involved in cell proliferation and migration makes it a potential target for future therapeutics.

Previous Section Next Section

Implications for future research and ECM as a therapeutic target

Despite the recent growth of information, many questions still remain, and continued research is required to build on and refine our current knowledge of the ECM, especially utilising the rapidly improving new technologies. The molecular nature of ECM-induced receptor complexes in the membrane and their movement upon activation can be monitored by methods such as single-molecule tracking using nanoparticles, fluorescence energy transfer technique or high-resolution live cell imaging. These studies will reveal more potential therapeutic opportunities in ECM remodelling. The caveat might be finding specific targets from the unique microenvironment of the diseased cells or tissues. Further investigations of the roles of ECM proteins in regulating signalling events would provide additional clues. However, multiple cell types and pathways within ECM are functionally interdependent and crosstalk to each other as described earlier, making it difficult to devise specific therapeutics that do not interfere with other pathways (Drucker et al. 2004). Nonetheless, multiple integrin antagonists have been tested as anti-tumour agents in clinical trials. Examples include αvβ3 and αvβ5 inhibitor cilengitide, which is currently being tested on glioblastoma patients in a phase III trial (Desgrosellier & Cheresh 2010). An excellent summary of recently developed novel agents targeting the tumour microenvironment can be found elsewhere (Hanna et al. 2009). ECM structural defects seem more difficult to treat, although the regenerative capacity of stem cells are being explored in different tissues; the problem encountered in recent attempts is that the injured microenvironment loses conformity with fibrotic scarring, thus resulting in a non-inducing environment where the stem cells cannot remodel (Berry et al. 2006). HSPGs should provide an interesting axis for novel approaches, since they act as master regulators of multiple ECM proteins and signalling pathways. In conclusion, ECM components are major molecular switches and crucial therapeutic targets to prevent abnormal growth factor receptor activities and to intervene in multiple signalling pathways, thus further investment could be made to aid the treatment and management of degenerative diseases, inflammation and cancer.

Previous Section Next Section

Declaration of interest

The authors declare that there is no conflict of interest that could be perceived as prejudicing the impartiality of the research reported.

Previous Section Next Section

Funding

This work was supported by Biotechnology and Biological Sciences Research Council Grant BB/F007167/1.

Received in final form 24 January 2011
Accepted 9 February 2011

© 2011 Society for Endocrinology

Previous Section

References

↵
1. Alam N,
2. Goel HL,
3. Zarif MJ,
4. Butterfield JE,
5. Perkins HM,
6. Sansoucy BG,
7. Sawyer TK &
8. Languino LR
2007 The integrin-growth factor receptor duet. Journal of Cellular Physiology 213 649–653doi:10.1002/jcp.21278.
CrossRef Medline Web of Science Google Scholar
↵
1. Allen BL &
2. Rapraeger AC
2003 Spatial and temporal expression of heparan sulfate in mouse development regulates FGF and FGF receptor assembly. Journal of Cell Biology 163 637–648doi:10.1083/jcb.200307053.
Abstract/FREE Full Text
↵
1. Apte SS,
2. Fukai N,
3. Beier DR &
4. Olsen BR
1997 The matrix metalloproteinase-14 (MMP-14) gene is structurally distinct from other MMP genes and is co-expressed with the TIMP-2 gene during mouse embryogenesis. Journal of Biological Chemistry 272 25511–25517doi:10.1074/jbc.272.41.25511.
Abstract/FREE Full Text
↵
1. Arias-Salgado EG,
2. Lizano S,
3. Sarkar S,
4. Brugge JS,
5. Ginsberg MH &
6. Shattil SJ
2003 Src kinase activation by direct interaction with the integrin beta cytoplasmic domain. PNAS 100 13298–13302doi:10.1073/pnas.2336149100.
Abstract/FREE Full Text
↵
1. Assoian RK &
2. Schwartz MA
2001 Coordinate signaling by integrins and receptor tyrosine kinases in the regulation of G1 phase cell-cycle progression. Current Opinion in Genetics and Development 11 48–53doi:10.1016/S0959-437X(00)00155-6.
CrossRef Medline Web of Science Google Scholar
↵
1. Baron V &
2. Schwartz M
2000 Cell adhesion regulates ubiquitin-mediated degradation of the platelet-derived growth factor receptor beta. Journal of Biological Chemistry 275 39318–39323doi:10.1074/jbc.M003618200.
Abstract/FREE Full Text
↵
1. Berry MF,
2. Engler AJ,
3. Woo YJ,
4. Pirolli TJ,
5. Bish LT,
6. Jayasankar V,
7. Morine KJ,
8. Gardner TJ,
9. Discher DE &
10. Sweeney HL
2006 Mesenchymal stem cell injection after myocardial infarction improves myocardial compliance. American Journal of Physiology. Heart and Circulatory Physiology 290 H2196–H2203doi:10.1152/ajpheart.01017.2005.
Abstract/FREE Full Text
↵
1. Bill HM,
2. Knudsen B,
3. Moores SL,
4. Muthuswamy SK,
5. Rao VR,
6. Brugge JS &
7. Miranti CK
2004 Epidermal growth factor receptor-dependent regulation of integrin-mediated signaling and cell cycle entry in epithelial cells. Molecular and Cellular Biology 24 8586–8599doi:10.1128/MCB.24.19.8586-8599.2004.
Abstract/FREE Full Text
↵
1. Blaber M,
2. DiSalvo J &
3. Thomas KA
1996 X-ray crystal structure of human acidic fibroblast growth factor. Biochemistry 35 2086–2094doi:10.1021/bi9521755.
CrossRef Medline Web of Science Google Scholar
↵
1. Blaine SA,
2. Ray KC,
3. Branch KM,
4. Robinson PS,
5. Whitehead RH &
6. Means AL
2009 Epidermal growth factor receptor regulates pancreatic fibrosis. American Journal of Physiology. Gastrointestinal and Liver Physiology 297 G434–G441doi:10.1152/ajpgi.00152.2009.
Abstract/FREE Full Text
↵
1. Brew K &
2. Nagase H
2010 The tissue inhibitors of metalloproteinases (TIMPs): an ancient family with structural and functional diversity. Biochimica et Biophysica Acta 1803 55–71doi:10.1016/j.bbamcr.2010.01.003.
CrossRef Medline Web of Science Google Scholar
↵
1. Brickman YG,
2. Ford MD,
3. Gallagher JT,
4. Nurcombe V,
5. Bartlett PF &
6. Turnbull JE
1998 Structural modification of fibroblast growth factor-binding heparan sulfate at a determinative stage of neural development. Journal of Biological Chemistry 273 4350–4359doi:10.1074/jbc.273.8.4350.
Abstract/FREE Full Text
↵
1. Brown MC,
2. Cary LA,
3. Jamieson JS,
4. Cooper JA &
5. Turner CE
2005 Src and FAK kinases cooperate to phosphorylate paxillin kinase linker, stimulate its focal adhesion localization, and regulate cell spreading and protrusiveness. Molecular Biology of the Cell 16 4316–4328doi:10.1091/mbc.E05-02-0131.
Abstract/FREE Full Text
↵
1. Brunner G,
2. Metz CN,
3. Nguyen H,
4. Gabrilove J,
5. Patel SR,
6. Davitz MA,
7. Rifkin DB &
8. Wilson EL
1994 An endogenous glycosylphosphatidylinositol-specific phospholipase D releases basic fibroblast growth factor-heparan sulfate proteoglycan complexes from human bone marrow cultures. Blood 83 2115–2125.
Abstract/FREE Full Text
↵
1. Casu B &
2. Lindahl U
2001 Structure and biological interactions of heparin and heparan sulfate. Advances in Carbohydrate Chemistry and Biochemistry 57 159–206doi:10.1016/S0065-2318(01)57017-1.
CrossRef Medline Web of Science Google Scholar
↵
1. Caswell PT,
2. Vadrevu S &
3. Norman JC
2009 Integrins: masters and slaves of endocytic transport. Nature Reviews. Molecular Cell Biology 10 843–853doi:10.1038/nrm2799.
CrossRef Medline Web of Science Google Scholar
↵
1. Chen CS,
2. Mrksich M,
3. Huang S,
4. Whitesides GM &
5. Ingber DE
1997 Geometric control of cell life and death. Science 276 1425–1428doi:10.1126/science.276.5317.1425.
Abstract/FREE Full Text
↵
1. Choi CK,
2. Vicente-Manzanares M,
3. Zareno J,
4. Whitmore LA,
5. Mogilner A &
6. Horwitz AR
2008 Actin and alpha-actinin orchestrate the assembly and maturation of nascent adhesions in a myosin II motor-independent manner. Nature Cell Biology 10 1039–1050doi:10.1038/ncb1763.
CrossRef Medline Web of Science Google Scholar
↵
1. Colige A,
2. Sieron AL,
3. Li SW,
4. Schwarze U,
5. Petty E,
6. Wertelecki W,
7. Wilcox W,
8. Krakow D,
9. Cohn DH,
10. Reardon W
11. et al.
1999 Human Ehlers–Danlos syndrome type VII C and bovine dermatosparaxis are caused by mutations in the procollagen I N-proteinase gene. American Journal of Human Genetics 65 308–317doi:10.1086/302504.
CrossRef Medline Web of Science Google Scholar
↵
1. Colognato H &
2. Yurchenco PD
2000 Form and function: the laminin family of heterotrimers. Developmental Dynamics 218 213–234doi:10.1002/(SICI)1097-0177(200006)218:2<213::AID-DVDY1>3.0.CO;2-R.
CrossRef Medline Web of Science Google Scholar
↵
1. Daoud J,
2. Petropavlovskaia M,
3. Rosenberg L &
4. Tabrizian M
2010 The effect of extracellular matrix components on the preservation of human islet function in vitro. Biomaterials 31 1676–1682doi:10.1016/j.biomaterials.2009.11.057.
CrossRef Medline Web of Science Google Scholar
↵
1. David G
1992 Structural and functional diversity of the heparan sulfate proteoglycans. Advances in Experimental Medicine and Biology 313 69–78.
CrossRef Medline Web of Science Google Scholar
↵
1. Day AJ &
2. Sheehan JK
2001 Hyaluronan: polysaccharide chaos to protein organisation. Current Opinion in Structural Biology 11 617–622doi:10.1016/S0959-440X(00)00256-6.
CrossRef Medline Web of Science Google Scholar
↵
1. Dempsey LA,
2. Brunn GJ &
3. Platt JL
2000 Heparanase, a potential regulator of cell–matrix interactions. Trends in Biochemical Sciences 25 349–351doi:10.1016/S0968-0004(00)01619-4.
CrossRef Medline Web of Science Google Scholar
↵
1. Desgrosellier JS &
2. Cheresh DA
2010 Integrins in cancer: biological implications and therapeutic opportunities. Nature Reviews. Cancer 10 9–22doi:10.1038/nrc2748.
CrossRef Medline Web of Science Google Scholar
↵
1. Discher DE,
2. Mooney DJ &
3. Zandstra PW
2009 Growth factors, matrices, and forces combine and control stem cells. Science 324 1673–1677doi:10.1126/science.1171643.
Abstract/FREE Full Text
↵
1. Drucker L,
2. Afensiev F,
3. Radnay J,
4. Shapira H &
5. Lishner M
2004 Co-administration of simvastatin and cytotoxic drugs is advantageous in myeloma cell lines. Anticancer Drugs 15 79–84doi:10.1097/00001813-200401000-00012.
CrossRef Medline Google Scholar
↵
1. Edin ML &
2. Juliano RL
2005 Raf-1 serine 338 phosphorylation plays a key role in adhesion-dependent activation of extracellular signal-regulated kinase by epidermal growth factor. Molecular and Cellular Biology 25 4466–4475doi:10.1128/MCB.25.11.4466-4475.2005.
Abstract/FREE Full Text
↵
1. Engler AJ,
2. Sen S,
3. Sweeney HL &
4. Discher DE
2006 Matrix elasticity directs stem cell lineage specification. Cell 126 677–689doi:10.1016/j.cell.2006.06.044.
CrossRef Medline Web of Science Google Scholar
↵
1. Esko JD &
2. Selleck SB
2002 Order out of chaos: assembly of ligand binding sites in heparan sulfate. Annual Review of Biochemistry 71 435–471doi:10.1146/annurev.biochem.71.110601.135458.
CrossRef Medline Web of Science Google Scholar
↵
1. Faham S,
2. Hileman RE,
3. Fromm JR,
4. Linhardt RJ &
5. Rees DC
1996 Heparin structure and interactions with basic fibroblast growth factor. Science 271 1116–1120doi:10.1126/science.271.5252.1116.
Abstract
↵
1. Friedl P &
2. Wolf K
2009 Proteolytic interstitial cell migration: a five-step process. Cancer Metastasis Reviews 28 129–135doi:10.1007/s10555-008-9174-3.
CrossRef Medline Web of Science Google Scholar
↵
1. Friedl A,
2. Chang Z,
3. Tierney A &
4. Rapraeger AC
1997 Differential binding of fibroblast growth factor-2 and -7 to basement membrane heparan sulfate: comparison of normal and abnormal human tissues. American Journal of Pathology 150 1443–1455.
Medline Web of Science Google Scholar
↵
1. Friedl A,
2. Filla M &
3. Rapraeger AC
2001 Tissue-specific binding by FGF and FGF receptors to endogenous heparan sulfates. Methods in Molecular Biology 171 535–546doi:10.1385/1-59259-209-0:535.
Medline Google Scholar
↵
1. Galbraith CG,
2. Yamada KM &
3. Sheetz MP
2002 The relationship between force and focal complex development. Journal of Cell Biology 159 695–705doi:10.1083/jcb.200204153.
Abstract/FREE Full Text
↵
1. Gao Y,
2. Xiao Q,
3. Ma H,
4. Li L,
5. Liu J,
6. Feng Y,
7. Fang Z,
8. Wu J,
9. Han X,
10. Zhang J
11. et al.
2010 LKB1 inhibits lung cancer progression through lysyl oxidase and extracellular matrix remodeling. PNAS 107 18892–18897doi:10.1073/pnas.1004952107.
Abstract/FREE Full Text
↵
1. Garcia AJ,
2. Coffinier C,
3. Larrain J,
4. Oelgeschlager M &
5. De Robertis EM
2002 Chordin-like CR domains and the regulation of evolutionarily conserved extracellular signaling systems. Gene 287 39–47doi:10.1016/S0378-1119(01)00827-7.
CrossRef Medline Web of Science Google Scholar
↵
1. Geiger B,
2. Bershadsky A,
3. Pankov R &
4. Yamada KM
2001 Transmembrane crosstalk between the extracellular matrix–cytoskeleton crosstalk. Nature Reviews. Molecular Cell Biology 2 793–805doi:10.1038/35099066.
CrossRef Medline Web of Science Google Scholar
↵
1. Geiger B,
2. Spatz JP &
3. Bershadsky AD
2009 Environmental sensing through focal adhesions. Nature Reviews. Molecular Cell Biology 10 21–33doi:10.1038/nrm2593.
CrossRef Medline Web of Science Google Scholar
↵
1. Goel HL,
2. Breen M,
3. Zhang J,
4. Das I,
5. Aznavoorian-Cheshire S,
6. Greenberg NM,
7. Elgavish A &
8. Languino LR
2005 beta1A integrin expression is required for type 1 insulin-like growth factor receptor mitogenic and transforming activities and localization to focal contacts. Cancer Research 65 6692–6700doi:10.1158/0008-5472.CAN-04-4315.
Abstract/FREE Full Text
↵
1. Grobe K &
2. Esko JD
2002 Regulated translation of heparan sulfate N-acetylglucosamine N-deacetylase/n-sulfotransferase isozymes by structured 5′-untranslated regions and internal ribosome entry sites. Journal of Biological Chemistry 277 30699–30706doi:10.1074/jbc.M111904200.
Abstract/FREE Full Text
↵
1. Guimond SE &
2. Turnbull JE
1999 Fibroblast growth factor receptor signalling is dictated by specific heparan sulphate saccharides. Current Biology 9 1343–1346doi:10.1016/S0960-9822(00)80060-3.
CrossRef Medline Web of Science Google Scholar
↵
1. Guimond SE,
2. Turnbull JE &
3. Yates EA
2006 Engineered bio-active polysaccharides from heparin. Macromolecular Bioscience 6 681–686doi:10.1002/mabi.200600042.
CrossRef Medline Web of Science Google Scholar
↵
1. Guimond SE,
2. Rudd TR,
3. Skidmore MA,
4. Ori A,
5. Gaudesi D,
6. Cosentino C,
7. Guerrini M,
8. Edge R,
9. Collison D,
10. McInnes E
11. et al.
2009 Cations modulate polysaccharide structure to determine FGF–FGFR signaling: a comparison of signaling and inhibitory polysaccharide interactions with FGF-1 in solution. Biochemistry 48 4772–4779doi:10.1021/bi802318z.
CrossRef Medline Web of Science Google Scholar
↵
1. Hanks SK,
2. Calalb MB,
3. Harper MC &
4. Patel SK
1992 Focal adhesion protein-tyrosine kinase phosphorylated in response to cell attachment to fibronectin. PNAS 89 8487–8491doi:10.1073/pnas.89.18.8487.
Abstract/FREE Full Text
↵
1. Hanna E,
2. Quick J &
3. Libutti SK
2009 The tumour microenvironment: a novel target for cancer therapy. Oral Disease 15 8–17doi:10.1111/j.1601-0825.2008.01471.x.
CrossRef Google Scholar
↵
1. Hardingham TE &
2. Fosang AJ
1992 Proteoglycans: many forms and many functions. FASEB Journal 6 861–870.
Abstract
↵
1. Hemler ME &
2. Lobb RR
1995 The leukocyte beta 1 integrins. Current Opinion in Hematology 2 61–67doi:10.1097/00062752-199502010-00009.
CrossRef Medline Google Scholar
↵
1. Hildebrand A,
2. Romaris M,
3. Rasmussen LM,
4. Heinegard D,
5. Twardzik DR,
6. Border WA &
7. Ruoslahti E
1994 Interaction of the small interstitial proteoglycans biglycan, decorin and fibromodulin with transforming growth factor beta. Biochemical Journal 302 527–534.
Abstract/FREE Full Text
↵
1. Hu Y,
2. Guimond SE,
3. Travers P,
4. Cadman SM,
5. Hohenester E,
6. Turnbull JE,
7. Kim SH &
8. Bouloux PMG
2009 Novel mechanisms of fibroblast growth factor receptor 1 regulation by extracellular matrix protein anosmin-1. Journal of Biological Chemistry 284 29905–29920doi:10.1074/jbc.M109.049155.
Abstract/FREE Full Text
↵
1. Hulett MD,
2. Freeman C,
3. Hamdorf BJ,
4. Baker RT,
5. Harris MJ &
6. Parish CR
1999 Cloning of mammalian heparanase, an important enzyme in tumor invasion and metastasis. Nature Medicine 5 803–809doi:10.1038/10525.
CrossRef Medline Web of Science Google Scholar
↵
1. Hulmes DJ
2002 Building collagen molecules, fibrils, and suprafibrillar structures. Journal of Structural Biology 137 2–10doi:10.1006/jsbi.2002.4450.
CrossRef Medline Web of Science Google Scholar
↵
1. Humphries JD,
2. Wang P,
3. Streuli C,
4. Geiger B,
5. Humphries MJ &
6. Ballestrem C
2007 Vinculin controls focal adhesion formation by direct interactions with talin and actin. Journal of Cell Biology 179 1043–1057doi:10.1083/jcb.200703036.
Abstract/FREE Full Text
↵
1. Ingber DE,
2. Madri JA &
3. Jamieson JD
1981 Role of basal lamina in neoplastic disorganization of tissue architecture. PNAS 78 3901–3905doi:10.1073/pnas.78.6.3901.
Abstract/FREE Full Text
↵
1. Jaffe AB &
2. Hall A
2005 Rho GTPases: biochemistry and biology. Annual Review of Cell and Development Biology 21 247–269doi:10.1146/annurev.cellbio.21.020604.150721.
CrossRef Google Scholar
↵
1. Jiang F,
2. Horber H,
3. Howard J &
4. Muller DJ
2004 Assembly of collagen into microribbons: effects of pH and electrolytes. Journal of Structural Biology 148 268–278doi:10.1016/j.jsb.2004.07.001.
CrossRef Medline Web of Science Google Scholar
↵
1. Kakkad SM,
2. Solaiyappan M,
3. O'Rourke B,
4. Stasinopoulos I,
5. Ackerstaff E,
6. Raman V,
7. Bhujwalla ZM &
8. Glunde K
2010 Hypoxic tumor microenvironments reduce collagen I fiber density. Neoplasia 12 608–617.
Medline Web of Science Google Scholar
↵
1. Kalluri R
2003 Basement membranes: structure, assembly and role in tumour angiogenesis. Nature Reviews. Cancer 3 422–433doi:10.1038/nrc1094.
CrossRef Medline Web of Science Google Scholar
↵
1. Kalluri R &
2. Zeisberg M
2006 Fibroblasts in cancer. Nature Reviews. Cancer 6 392–401doi:10.1038/nrc1877.
CrossRef Medline Web of Science Google Scholar
↵
1. Kamei N,
2. Kwon SM,
3. Alev C,
4. Ishikawa M,
5. Yokoyama A,
6. Nakanishi K,
7. Yamada K,
8. Horii M,
9. Nishimura H,
10. Takaki S
11. et al.
2010 Lnk deletion reinforces the function of bone marrow progenitors in promoting neovascularization and astrogliosis following spinal cord injury. Stem Cells 28 365–375doi:10.1002/stem.243.
Medline Web of Science Google Scholar
↵
1. Kan M,
2. Wang F,
3. Xu J,
4. Crabb JW,
5. Hou J &
6. McKeehan WL
1993 An essential heparin-binding domain in the fibroblast growth factor receptor kinase. Science 259 1918–1921doi:10.1126/science.8456318.
Abstract/FREE Full Text
↵
1. Kenny PA &
2. Bissell MJ
2003 Tumor reversion: correction of malignant behavior by microenvironmental cues. International Journal of Cancer 107 688–695doi:10.1002/ijc.11491.
CrossRef Medline Web of Science Google Scholar
↵
1. Kielty CM,
2. Sherratt MJ &
3. Shuttleworth CA
2002 Elastic fibres. Journal of Cell Science 115 2817–2828.
Abstract/FREE Full Text
↵
1. Kim SH &
2. Kim SH
2008 Antagonistic effect of EGF on FAK phosphorylation/dephosphorylation in a cell. Cell Biochemistry and Function 26 539–547doi:10.1002/cbf.1457.
CrossRef Medline Web of Science Google Scholar
↵
1. Kirkpatrick CA,
2. Dimitroff BD,
3. Rawson JM &
4. Selleck SB
2004 Spatial regulation of Wingless morphogen distribution and signaling by Dally-like protein. Developmental Cell 7 513–523doi:10.1016/j.devcel.2004.08.004.
CrossRef Medline Web of Science Google Scholar
↵
1. Kiselyov VV,
2. Skladchikova G,
3. Hinsby AM,
4. Jensen PH,
5. Kulahin N,
6. Soroka V,
7. Pedersen N,
8. Tsetlin V,
9. Poulsen FM,
10. Berezin V
11. et al.
2003 Structural basis for a direct interaction between FGFR1 and NCAM and evidence for a regulatory role of ATP. Structure 11 691–701doi:10.1016/S0969-2126(03)00096-0.
CrossRef Medline Google Scholar
↵
1. Kjellen L &
2. Lindahl U
1991 Proteoglycans: structures and interactions. Annual Review of Biochemistry 60 443–475doi:10.1146/annurev.bi.60.070191.002303.
CrossRef Medline Web of Science Google Scholar
↵
1. Knecht M
1988 Plasminogen activator is associated with the extracellular matrix of ovarian granulosa cells. Molecular and Cellular Endocrinology 56 1–9doi:10.1016/0303-7207(88)90002-0.
CrossRef Medline Web of Science Google Scholar
↵
1. Kresse H &
2. Schonherr E
2001 Proteoglycans of the extracellular matrix and growth control. Journal of Cellular Physiology 189 266–274doi:10.1002/jcp.10030.
CrossRef Medline Web of Science Google Scholar
↵
1. Kreuger J,
2. Perez L,
3. Giraldez AJ &
4. Cohen SM
2004 Opposing activities of Dally-like glypican at high and low levels of Wingless morphogen activity. Developmental Cell 7 503–512doi:10.1016/j.devcel.2004.08.005.
CrossRef Medline Web of Science Google Scholar
↵
1. van Kuppevelt TH,
2. Dennissen MA,
3. van Venrooij WJ,
4. Hoet RM &
5. Veerkamp JH
1998 Generation and application of type-specific anti-heparan sulfate antibodies using phage display technology. Further evidence for heparan sulfate heterogeneity in the kidney. Journal of Biological Chemistry 273 12960–12966doi:10.1074/jbc.273.21.12960.
Abstract/FREE Full Text
↵
1. Lamanna WC,
2. Baldwin RJ,
3. Padva M,
4. Kalus I,
5. Ten DG,
6. van Kuppevelt TH,
7. Gallagher JT,
8. von FK,
9. Dierks T &
10. Merry CL
2006 Heparan sulfate 6-O-endosulfatases: discrete in vivo activities and functional co-operativity. Biochemical Journal 400 63–73doi:10.1042/BJ20060848.
Abstract/FREE Full Text
↵
1. Legate KR,
2. Wickstrom SA &
3. Fassler R
2009 Genetic and cell biological analysis of integrin outside-in signaling. Genes and Development 23 397–418doi:10.1101/gad.1758709.
Abstract/FREE Full Text
↵
1. Li JP &
2. Vlodavsky I
2009 Heparin, heparan sulfate and heparanase in inflammatory reactions. Thrombosis and Haemostasis 102 823–828doi:10.1160/TH09-02-0091.
Medline Web of Science Google Scholar
↵
1. Lindahl U,
2. Kusche M,
3. Lidholt K &
4. Oscarsson LG
1989 Biosynthesis of heparin and heparan sulfate. Annals of the New York Academy of Sciences 556 36–50doi:10.1111/j.1749-6632.1989.tb22488.x.
CrossRef Medline Web of Science Google Scholar
↵
1. Lock R &
2. Debnath J
2008 Extracellular matrix regulation of autophagy. Current Opinion in Cell Biology 20 583–588doi:10.1016/j.ceb.2008.05.002.
CrossRef Medline Web of Science Google Scholar
↵
1. Maffini MV,
2. Soto AM,
3. Calabro JM,
4. Ucci AA &
5. Sonnenschein C
2004 The stroma as a crucial target in rat mammary gland carcinogenesis. Journal of Cell Science 117 1495–1502doi:10.1242/jcs.01000.
Abstract/FREE Full Text
↵
1. Maffini MV,
2. Calabro JM,
3. Soto AM &
4. Sonnenschein C
2005 Stromal regulation of neoplastic development: age-dependent normalization of neoplastic mammary cells by mammary stroma. American Journal of Pathology 167 1405–1410doi:10.1016/S0002-9440(10)61227-8.
CrossRef Medline Web of Science Google Scholar
↵
1. Manon-Jensen T,
2. Itoh Y &
3. Couchman JR
2010 Proteoglycans in health and disease: the multiple roles of syndecan shedding. FEBS Journal 277 3876–3889doi:10.1111/j.1742-4658.2010.07798.x.
CrossRef Medline Web of Science Google Scholar
↵
1. Marastoni S,
2. Ligresti G,
3. Lorenzon E,
4. Colombatti A &
5. Mongiat M
2008 Extracellular matrix: a matter of life and death. Connective Tissue Research 49 203–206doi:10.1080/03008200802143190.
CrossRef Medline Web of Science Google Scholar
↵
1. Mitra SK,
2. Hanson DA &
3. Schlaepfer DD
2005 Focal adhesion kinase: in command and control of cell motility. Nature Reviews. Molecular Cell Biology 6 56–68doi:10.1038/nrm1549.
CrossRef Medline Web of Science Google Scholar
↵
1. Moser M,
2. Nieswandt B,
3. Ussar S,
4. Pozgajova M &
5. Fassler R
2008 Kindlin-3 is essential for integrin activation and platelet aggregation. Nature Medicine 14 325–330doi:10.1038/nm1722.
CrossRef Medline Web of Science Google Scholar
↵
1. Mott JD &
2. Werb Z
2004 Regulation of matrix biology by matrix metalloproteinases. Current Opinion in Cell Biology 16 558–564doi:10.1016/j.ceb.2004.07.010.
CrossRef Medline Web of Science Google Scholar
↵
1. Mundhenke C,
2. Meyer K,
3. Drew S &
4. Friedl A
2002 Heparan sulfate proteoglycans as regulators of fibroblast growth factor-2 receptor binding in breast carcinomas. American Journal of Pathology 160 185–194doi:10.1016/S0002-9440(10)64362-3.
CrossRef Medline Web of Science Google Scholar
↵
1. Nagai N,
2. Habuchi H,
3. Esko JD &
4. Kimata K
2004 Stem domains of heparan sulfate 6-O-sulfotransferase are required for Golgi localization, oligomer formation and enzyme activity. Journal of Cell Science 117 3331–3341doi:10.1242/jcs.01191.
Abstract/FREE Full Text
↵
1. Narita K,
2. Staub J,
3. Chien J,
4. Meyer K,
5. Bauer M,
6. Friedl A,
7. Ramakrishnan S &
8. Shridhar V
2006 HSulf-1 inhibits angiogenesis and tumorigenesis in vivo. Cancer Research 66 6025–6032doi:10.1158/0008-5472.CAN-05-3582.
Abstract/FREE Full Text
↵
1. Ori A,
2. Free P,
3. Courty J,
4. Wilkinson MC &
5. Fernig DG
2009 Identification of heparin-binding sites in proteins by selective labeling. Molecular and Cellular Proteomics 8 2256–2265doi:10.1074/mcp.M900031-MCP200.
CrossRef Google Scholar
↵
1. Ornitz DM,
2. Xu J,
3. Colvin JS,
4. McEwen DG,
5. MacArthur CA,
6. Coulier F,
7. Gao G &
8. Goldfarb M
1996 Receptor specificity of the fibroblast growth factor family. Journal of Biological Chemistry 271 15292–15297doi:10.1074/jbc.271.25.15292.
Abstract/FREE Full Text
↵
1. Overall CM &
2. Lopez-Otin C
2002 Strategies for MMP inhibition in cancer: innovations for the post-trial era. Nature Reviews. Cancer 2 657–672doi:10.1038/nrc884.
CrossRef Medline Web of Science Google Scholar
↵
1. Park JH,
2. Ryu JM &
3. Han HJ
2011 Involvement of caveolin-1 in fibronectin-induced mouse embryonic stem cell proliferation: role of FAK, RhoA, PI3K/Akt, and ERK 1/2 pathways. Journal of Cellular Physiology 226 267–275doi:10.1002/jcp.22338.
CrossRef Medline Web of Science Google Scholar
↵
1. Patel VN,
2. Knox SM,
3. Likar KM,
4. Lathrop CA,
5. Hossain R,
6. Eftekhari S,
7. Whitelock JM,
8. Elkin M,
9. Vlodavsky I &
10. Hoffman MP
2007 Heparanase cleavage of perlecan heparan sulfate modulates FGF10 activity during ex vivo submandibular gland branching morphogenesis. Development 134 4177–4186doi:10.1242/dev.011171.
Abstract/FREE Full Text
↵
1. Pelham RJ Jr. &
2. Wang Y
1997 Cell locomotion and focal adhesions are regulated by substrate flexibility. PNAS 94 13661–13665doi:10.1073/pnas.94.25.13661.
Abstract/FREE Full Text
↵
1. Pinhal MA,
2. Smith B,
3. Olson S,
4. Aikawa J,
5. Kimata K &
6. Esko JD
2001 Enzyme interactions in heparan sulfate biosynthesis: uronosyl 5-epimerase and 2-O-sulfotransferase interact in vivo. PNAS 98 12984–12989doi:10.1073/pnas.241175798.
Abstract/FREE Full Text
↵
1. del Pozo MA,
2. Alderson NB,
3. Kiosses WB,
4. Chiang HH,
5. Anderson RG &
6. Schwartz MA
2004 Integrins regulate Rac targeting by internalization of membrane domains. Science 303 839–842doi:10.1126/science.1092571.
Abstract/FREE Full Text
↵
1. Preissner KT &
2. Seiffert D
1998 Role of vitronectin and its receptors in haemostasis and vascular remodeling. Thrombosis Research 89 1–21doi:10.1016/S0049-3848(97)00298-3.
CrossRef Medline Web of Science Google Scholar
↵
1. Robinson CJ &
2. Stringer SE
2001 The splice variants of vascular endothelial growth factor (VEGF) and their receptors. Journal of Cell Science 114 853–865.
Abstract/FREE Full Text
↵
1. Rudd TR,
2. Skidmore MA,
3. Guimond SE,
4. Guerrini M,
5. Cosentino C,
6. Edge R,
7. Brown A,
8. Clarke DT,
9. Torri G,
10. Turnbull JE
11. et al.
2008 Site-specific interactions of copper(II) ions with heparin revealed with complementary (SRCD, NMR, FTIR and EPR) spectroscopic techniques. Carbohydrate Research 343 2184–2193doi:10.1016/j.carres.2007.12.019.
CrossRef Medline Web of Science Google Scholar
↵
1. Ruhrberg C,
2. Gerhardt H,
3. Golding M,
4. Watson R,
5. Ioannidou S,
6. Fujisawa H,
7. Betsholtz C &
8. Shima DT
2002 Spatially restricted patterning cues provided by heparin-binding VEGF-A control blood vessel branching morphogenesis. Genes and Development 16 2684–2698doi:10.1101/gad.242002.
Abstract/FREE Full Text
↵
1. Ruoslahti E
1988 Fibronectin and its receptors. Annual Review of Biochemistry 57 375–413doi:10.1146/annurev.bi.57.070188.002111.
CrossRef Medline Web of Science Google Scholar
↵
1. Ruoslahti E
1996 RGD and other recognition sequences for integrins. Annual Review of Cell and Development Biology 12 697–715doi:10.1146/annurev.cellbio.12.1.697.
CrossRef Google Scholar
↵
1. Ruoslahti E
2002 Specialization of tumour vasculature. Nature Reviews. Cancer 2 83–90doi:10.1038/nrc724.
CrossRef Medline Web of Science Google Scholar
↵
1. Salanueva IJ,
2. Cerezo A,
3. Guadamillas MC &
4. del Pozo MA
2007 Integrin regulation of caveolin function. Journal of Cellular and Molecular Medicine 11 969–980doi:10.1111/j.1582-4934.2007.00109.x.
CrossRef Medline Web of Science Google Scholar
↵
1. Scaffidi AK,
2. Petrovic N,
3. Moodley YP,
4. Fogel-Petrovic M,
5. Kroeger KM,
6. Seeber RM,
7. Eidne KA,
8. Thompson PJ &
9. Knight DA
2004 alpha(v)beta(3) Integrin interacts with the transforming growth factor beta (TGFbeta) type II receptor to potentiate the proliferative effects of TGFbeta1 in living human lung fibroblasts. Journal of Biological Chemistry 279 37726–37733doi:10.1074/jbc.M403010200.
Abstract/FREE Full Text
↵
1. Schenk S,
2. Hintermann E,
3. Bilban M,
4. Koshikawa N,
5. Hojilla C,
6. Khokha R &
7. Quaranta V
2003 Binding to EGF receptor of a laminin-5 EGF-like fragment liberated during MMP-dependent mammary gland involution. Journal of Cell Biology 161 197–209doi:10.1083/jcb.200208145.
Abstract/FREE Full Text
↵
1. Schneller M,
2. Vuori K &
3. Ruoslahti E
1997 Alphavbeta3 integrin associates with activated insulin and PDGFbeta receptors and potentiates the biological activity of PDGF. EMBO Journal 16 5600–5607doi:10.1093/emboj/16.18.5600.
Abstract
↵
1. Shiomi T,
2. Lemaitre V,
3. D'Armiento J &
4. Okada Y
2010 Matrix metalloproteinases, a disintegrin and metalloproteinases, and a disintegrin and metalloproteinases with thrombospondin motifs in non-neoplastic diseases. Pathology International 60 477–496doi:10.1111/j.1440-1827.2010.02547.x.
CrossRef Medline Web of Science Google Scholar
↵
1. Skidmore MA,
2. Guimond SE,
3. Rudd TR,
4. Fernig DG,
5. Turnbull JE &
6. Yates EA
2008 The activities of heparan sulfate and its analogue heparin are dictated by biosynthesis, sequence, and conformation. Connective Tissue Research 49 140–144doi:10.1080/03008200802148595.
CrossRef Medline Web of Science Google Scholar
↵
1. Skinner MK,
2. Tung PS &
3. Fritz IB
1985 Cooperativity between Sertoli cells and testicular peritubular cells in the production and deposition of extracellular matrix components. Journal of Cell Biology 100 1941–1947doi:10.1083/jcb.100.6.1941.
Abstract/FREE Full Text
↵
1. Slack-Davis JK,
2. Eblen ST,
3. Zecevic M,
4. Boerner SA,
5. Tarcsafalvi A,
6. Diaz HB,
7. Marshall MS,
8. Weber MJ,
9. Parsons JT &
10. Catling AD
2003 PAK1 phosphorylation of MEK1 regulates fibronectin-stimulated MAPK activation. Journal of Cell Biology 162 281–291doi:10.1083/jcb.200212141.
Abstract/FREE Full Text
↵
1. Sood AK,
2. Armaiz-Pena GN,
3. Halder J,
4. Nick AM,
5. Stone RL,
6. Hu W,
7. Carroll AR,
8. Spannuth WA,
9. Deavers MT,
10. Allen JK
11. et al.
2010 Adrenergic modulation of focal adhesion kinase protects human ovarian cancer cells from anoikis. Journal of Clinical Investigation 120 1515–1523doi:10.1172/JCI40802.
CrossRef Medline Web of Science Google Scholar
↵
1. Sridhar SC &
2. Miranti CK
2006 Tetraspanin KAI1/CD82 suppresses invasion by inhibiting integrin-dependent crosstalk with c-Met receptor and Src kinases. Oncogene 25 2367–2378doi:10.1038/sj.onc.1209269.
CrossRef Medline Web of Science Google Scholar
↵
1. Sternlicht MD,
2. Lochter A,
3. Sympson CJ,
4. Huey B,
5. Rougier JP,
6. Gray JW,
7. Pinkel D,
8. Bissell MJ &
9. Werb Z
1999 The stromal proteinase MMP3/stromelysin-1 promotes mammary carcinogenesis. Cell 98 137–146doi:10.1016/S0092-8674(00)81009-0.
CrossRef Medline Web of Science Google Scholar
↵
1. Tadokoro S,
2. Shattil SJ,
3. Eto K,
4. Tai V,
5. Liddington RC,
6. de Pereda JM,
7. Ginsberg MH &
8. Calderwood DA
2003 Talin binding to integrin beta tails: a final common step in integrin activation. Science 302 103–106doi:10.1126/science.1086652.
Abstract/FREE Full Text
↵
1. Tang BL
2001 ADAMTS: a novel family of extracellular matrix proteases. International Journal of Biochemistry and Cell Biology 33 33–44doi:10.1016/S1357-2725(00)00061-3.
CrossRef Medline Web of Science Google Scholar
↵
1. Thrailkill KM,
2. Clay BR &
3. Fowlkes JL
2009 Matrix metalloproteinases: their potential role in the pathogenesis of diabetic nephropathy. Endocrine 35 1–10doi:10.1007/s12020-008-9114-6.
CrossRef Medline Web of Science Google Scholar
↵
1. Tilghman RW &
2. Parsons JT
2008 Focal adhesion kinase as a regulator of cell tension in the progression of cancer. Seminars in Cancer Biology 18 45–52doi:10.1016/j.semcancer.2007.08.002.
CrossRef Medline Web of Science Google Scholar
↵
1. Tortorella MD,
2. Burn TC,
3. Pratta MA,
4. Abbaszade I,
5. Hollis JM,
6. Liu R,
7. Rosenfeld SA,
8. Copeland RA,
9. Decicco CP,
10. Wynn R
11. et al.
1999 Purification and cloning of aggrecanase-1: a member of the ADAMTS family of proteins. Science 284 1664–1666doi:10.1126/science.284.5420.1664.
Abstract/FREE Full Text
↵
1. Turnbull JE &
2. Gallagher JT
1990 Molecular organization of heparan sulphate from human skin fibroblasts. Biochemical Journal 265 715–724.
Abstract/FREE Full Text
↵
1. Turnbull JE,
2. Hopwood JJ &
3. Gallagher JT
1999 A strategy for rapid sequencing of heparan sulfate and heparin saccharides. PNAS 96 2698–2703doi:10.1073/pnas.96.6.2698.
Abstract/FREE Full Text
↵
1. Vincent TL,
2. McLean CJ,
3. Full LE,
4. Peston D &
5. Saklatvala J
2007 FGF-2 is bound to perlecan in the pericellular matrix of articular cartilage, where it acts as a chondrocyte mechanotransducer. Osteoarthritis and Cartilage 15 752–763doi:10.1016/j.joca.2007.01.021.
CrossRef Medline Web of Science Google Scholar
↵
1. Vlodavsky I,
2. Friedmann Y,
3. Elkin M,
4. Aingorn H,
5. Atzmon R,
6. Ishai-Michaeli R,
7. Bitan M,
8. Pappo O,
9. Peretz T,
10. Michal I
11. et al.
1999 Mammalian heparanase: gene cloning, expression and function in tumor progression and metastasis. Nature Medicine 5 793–802doi:10.1038/10518.
CrossRef Medline Web of Science Google Scholar
↵
1. Wang X,
2. Harris RE,
3. Bayston LJ &
4. Ashe HL
2008 Type IV collagens regulate BMP signalling in Drosophila. Nature 455 72–77doi:10.1038/nature07214.
CrossRef Medline Web of Science Google Scholar
↵
1. Weaver VM,
2. Petersen OW,
3. Wang F,
4. Larabell CA,
5. Briand P,
6. Damsky C &
7. Bissell MJ
1997 Reversion of the malignant phenotype of human breast cells in three-dimensional culture and in vivo by integrin blocking antibodies. Journal of Cell Biology 137 231–245doi:10.1083/jcb.137.1.231.
Abstract/FREE Full Text
↵
1. Weaver A,
2. Goncalves da SA,
3. Nuttall RK,
4. Edwards DR,
5. Shapiro SD,
6. Rivest S &
7. Yong VW
2005 An elevated matrix metalloproteinase (MMP) in an animal model of multiple sclerosis is protective by affecting Th1/Th2 polarization. FASEB Journal 19 1668–1670.
Abstract/FREE Full Text
↵
1. Wells RG
2008 The role of matrix stiffness in regulating cell behavior. Hepatology 47 1394–1400doi:10.1002/hep.22193.
CrossRef Medline Web of Science Google Scholar
↵
1. Wells JE,
2. Hurlbert RJ,
3. Fehlings MG &
4. Yong VW
2003 Neuroprotection by minocycline facilitates significant recovery from spinal cord injury in mice. Brain 126 1628–1637doi:10.1093/brain/awg178.
Abstract/FREE Full Text
↵
1. White DE &
2. Muller WJ
2007 Multifaceted roles of integrins in breast cancer metastasis. Journal of Mammary Gland Biology and Neoplasia 12 135–142doi:10.1007/s10911-007-9045-5.
CrossRef Medline Web of Science Google Scholar
↵
1. Whitelock JM,
2. Melrose J &
3. Iozzo RV
2008 Diverse cell signaling events modulated by perlecan. Biochemistry 47 11174–11183doi:10.1021/bi8013938.
CrossRef Medline Web of Science Google Scholar
↵
1. Wijelath ES,
2. Rahman S,
3. Namekata M,
4. Murray J,
5. Nishimura T,
6. Mostafavi-Pour Z,
7. Patel Y,
8. Suda Y,
9. Humphries MJ &
10. Sobel M
2006 Heparin-II domain of fibronectin is a vascular endothelial growth factor-binding domain: enhancement of VEGF biological activity by a singular growth factor/matrix protein synergism. Circulation Research 99 853–860doi:10.1161/01.RES.0000246849.17887.66.
Abstract/FREE Full Text
↵
1. Wiseman BS &
2. Werb Z
2002 Stromal effects on mammary gland development and breast cancer. Science 296 1046–1049doi:10.1126/science.1067431.
Abstract/FREE Full Text
↵
1. Wong P,
2. Hampton B,
3. Szylobryt E,
4. Gallagher AM,
5. Jaye M &
6. Burgess WH
1995 Analysis of putative heparin-binding domains of fibroblast growth factor-1. Using site-directed mutagenesis and peptide analogues. Journal of Biological Chemistry 270 25805–25811doi:10.1074/jbc.270.43.25805.
Abstract/FREE Full Text
↵
1. Yang N,
2. Mosher R,
3. Seo S,
4. Beebe D &
5. Friedl A
2011 Syndecan-1 in breast cancer stroma fibroblasts regulates extracellular matrix fiber organization and carcinoma cell motility. American Journal of Pathology 178 325–335doi:10.1016/j.ajpath.2010.11.039.
CrossRef Medline Web of Science Google Scholar
↵
1. Yodoi R,
2. Tamba S,
3. Morimoto K,
4. Segi-Nishida E,
5. Nishihara M,
6. Ichikawa A,
7. Narumiya S &
8. Sugimoto Y
2009 RhoA/Rho kinase signaling in the cumulus mediates extracellular matrix assembly. Endocrinology 150 3345–3352doi:10.1210/en.2008-1449.
CrossRef Medline Web of Science Google Scholar
↵
1. Yong VW
2005 Metalloproteinases: mediators of pathology and regeneration in the CNS. Nature Reviews. Neuroscience 6 931–944doi:10.1038/nrn1807.
CrossRef Medline Web of Science Google Scholar
↵
1. Yu X,
2. Miyamoto S &
3. Mekada E
2000 Integrin alpha 2 beta 1-dependent EGF receptor activation at cell–cell contact sites. Journal of Cell Science 113 2139–2147.
Abstract/FREE Full Text
↵
1. Yu WH,
2. Woessner JF Jr.,
3. McNeish JD &
4. Stamenkovic I
2002 CD44 anchors the assembly of matrilysin/MMP-7 with heparin-binding epidermal growth factor precursor and ErbB4 and regulates female reproductive organ remodeling. Genes and Development 16 307–323doi:10.1101/gad.925702.
Abstract/FREE Full Text
↵
1. Zaidel-Bar R,
2. Itzkovitz S,
3. Ma'ayan A,
4. Iyengar R &
5. Geiger B
2007 Functional atlas of the integrin adhesome. Nature Cell Biology 9 858–867doi:10.1038/ncb0807-858.
CrossRef Medline Web of Science Google Scholar
↵
1. Zcharia E,
2. Zilka R,
3. Yaar A,
4. Yacoby-Zeevi O,
5. Zetser A,
6. Metzger S,
7. Sarid R,
8. Naggi A,
9. Casu B,
10. Ilan N
11. et al.
2005 Heparanase accelerates wound angiogenesis and wound healing in mouse and rat models. FASEB Journal 19 211–221doi:10.1096/fj.04-1970com.
Abstract/FREE Full Text
↵
1. Zhang X &
2. Yee D
2000 Tyrosine kinase signalling in breast cancer: insulin-like growth factors and their receptors in breast cancer. Breast Cancer Research 2 170–175doi:10.1186/bcr50.
CrossRef Medline Web of Science Google Scholar

[1] ↵

Alam N,

Goel HL,

Zarif MJ,

Butterfield JE,

Perkins HM,

Sansoucy BG,

Sawyer TK &

Languino LR

2007 The integrin-growth factor receptor duet. Journal of Cellular Physiology 213 649–653doi:10.1002/jcp.21278.

CrossRef Medline Web of Science Google Scholar

[2] Alam N,

[3] Goel HL,

[4] Zarif MJ,

[5] Butterfield JE,

[6] Perkins HM,

[7] Sansoucy BG,

[8] Sawyer TK &

[9] Languino LR

[10] ↵

Allen BL &

Rapraeger AC

2003 Spatial and temporal expression of heparan sulfate in mouse development regulates FGF and FGF receptor assembly. Journal of Cell Biology 163 637–648doi:10.1083/jcb.200307053.

Abstract/FREE Full Text

[11] Allen BL &

[12] Rapraeger AC

[13] ↵

Apte SS,

Fukai N,

Beier DR &

Olsen BR

1997 The matrix metalloproteinase-14 (MMP-14) gene is structurally distinct from other MMP genes and is co-expressed with the TIMP-2 gene during mouse embryogenesis. Journal of Biological Chemistry 272 25511–25517doi:10.1074/jbc.272.41.25511.

Abstract/FREE Full Text

[14] Apte SS,

[15] Fukai N,

[16] Beier DR &

[17] Olsen BR

[18] ↵

Arias-Salgado EG,

Lizano S,

Sarkar S,

Brugge JS,

Ginsberg MH &

Shattil SJ

2003 Src kinase activation by direct interaction with the integrin beta cytoplasmic domain. PNAS 100 13298–13302doi:10.1073/pnas.2336149100.

Abstract/FREE Full Text

[19] Arias-Salgado EG,

[20] Lizano S,

[21] Sarkar S,

[22] Brugge JS,

[23] Ginsberg MH &

[24] Shattil SJ

[25] ↵

Assoian RK &

Schwartz MA

2001 Coordinate signaling by integrins and receptor tyrosine kinases in the regulation of G1 phase cell-cycle progression. Current Opinion in Genetics and Development 11 48–53doi:10.1016/S0959-437X(00)00155-6.

CrossRef Medline Web of Science Google Scholar

[26] Assoian RK &

[27] Schwartz MA

[28] ↵

Baron V &

Schwartz M

2000 Cell adhesion regulates ubiquitin-mediated degradation of the platelet-derived growth factor receptor beta. Journal of Biological Chemistry 275 39318–39323doi:10.1074/jbc.M003618200.

Abstract/FREE Full Text

[29] Baron V &

[30] Schwartz M

[31] ↵

Berry MF,

Engler AJ,

Woo YJ,

Pirolli TJ,

Bish LT,

Jayasankar V,

Morine KJ,

Gardner TJ,

Discher DE &

Sweeney HL

2006 Mesenchymal stem cell injection after myocardial infarction improves myocardial compliance. American Journal of Physiology. Heart and Circulatory Physiology 290 H2196–H2203doi:10.1152/ajpheart.01017.2005.

Abstract/FREE Full Text

[32] Berry MF,

[33] Engler AJ,

[34] Woo YJ,

[35] Pirolli TJ,

[36] Bish LT,

[37] Jayasankar V,

[38] Morine KJ,

[39] Gardner TJ,

[40] Discher DE &

[41] Sweeney HL

[42] ↵

Bill HM,

Knudsen B,

Moores SL,

Muthuswamy SK,

Rao VR,

Brugge JS &

Miranti CK

2004 Epidermal growth factor receptor-dependent regulation of integrin-mediated signaling and cell cycle entry in epithelial cells. Molecular and Cellular Biology 24 8586–8599doi:10.1128/MCB.24.19.8586-8599.2004.

Abstract/FREE Full Text

[43] Bill HM,

[44] Knudsen B,

[45] Moores SL,

[46] Muthuswamy SK,

[47] Rao VR,

[48] Brugge JS &

[49] Miranti CK

[50] ↵

Blaber M,

DiSalvo J &

Thomas KA

1996 X-ray crystal structure of human acidic fibroblast growth factor. Biochemistry 35 2086–2094doi:10.1021/bi9521755.

CrossRef Medline Web of Science Google Scholar

[51] Blaber M,

[52] DiSalvo J &

[53] Thomas KA

[54] ↵

Blaine SA,

Ray KC,

Branch KM,

Robinson PS,

Whitehead RH &

Means AL

2009 Epidermal growth factor receptor regulates pancreatic fibrosis. American Journal of Physiology. Gastrointestinal and Liver Physiology 297 G434–G441doi:10.1152/ajpgi.00152.2009.

Abstract/FREE Full Text

[55] Blaine SA,

[56] Ray KC,

[57] Branch KM,

[58] Robinson PS,

[59] Whitehead RH &

[60] Means AL

[61] ↵

Brew K &

Nagase H

2010 The tissue inhibitors of metalloproteinases (TIMPs): an ancient family with structural and functional diversity. Biochimica et Biophysica Acta 1803 55–71doi:10.1016/j.bbamcr.2010.01.003.

CrossRef Medline Web of Science Google Scholar

[62] Brew K &

[63] Nagase H

[64] ↵

Brickman YG,

Ford MD,

Gallagher JT,

Nurcombe V,

Bartlett PF &

Turnbull JE

1998 Structural modification of fibroblast growth factor-binding heparan sulfate at a determinative stage of neural development. Journal of Biological Chemistry 273 4350–4359doi:10.1074/jbc.273.8.4350.

Abstract/FREE Full Text

[65] Brickman YG,

[66] Ford MD,

[67] Gallagher JT,

[68] Nurcombe V,

[69] Bartlett PF &

[70] Turnbull JE

[71] ↵

Brown MC,

Cary LA,

Jamieson JS,

Cooper JA &

Turner CE

2005 Src and FAK kinases cooperate to phosphorylate paxillin kinase linker, stimulate its focal adhesion localization, and regulate cell spreading and protrusiveness. Molecular Biology of the Cell 16 4316–4328doi:10.1091/mbc.E05-02-0131.

Abstract/FREE Full Text

[72] Brown MC,

[73] Cary LA,

[74] Jamieson JS,

[75] Cooper JA &

[76] Turner CE

[77] ↵

Brunner G,

Metz CN,

Nguyen H,

Gabrilove J,

Patel SR,

Davitz MA,

Rifkin DB &

Wilson EL

1994 An endogenous glycosylphosphatidylinositol-specific phospholipase D releases basic fibroblast growth factor-heparan sulfate proteoglycan complexes from human bone marrow cultures. Blood 83 2115–2125.

Abstract/FREE Full Text

[78] Brunner G,

[79] Metz CN,

[80] Nguyen H,

[81] Gabrilove J,

[82] Patel SR,

[83] Davitz MA,

[84] Rifkin DB &

[85] Wilson EL

[86] ↵

Casu B &

Lindahl U

2001 Structure and biological interactions of heparin and heparan sulfate. Advances in Carbohydrate Chemistry and Biochemistry 57 159–206doi:10.1016/S0065-2318(01)57017-1.

CrossRef Medline Web of Science Google Scholar

[87] Casu B &

[88] Lindahl U

[89] ↵

Caswell PT,

Vadrevu S &

Norman JC

2009 Integrins: masters and slaves of endocytic transport. Nature Reviews. Molecular Cell Biology 10 843–853doi:10.1038/nrm2799.

CrossRef Medline Web of Science Google Scholar

[90] Caswell PT,

[91] Vadrevu S &

[92] Norman JC

[93] ↵

Chen CS,

Mrksich M,

Huang S,

Whitesides GM &

Ingber DE

1997 Geometric control of cell life and death. Science 276 1425–1428doi:10.1126/science.276.5317.1425.

Abstract/FREE Full Text

[94] Chen CS,

[95] Mrksich M,

[96] Huang S,

[97] Whitesides GM &

[98] Ingber DE

[99] ↵

Choi CK,

Vicente-Manzanares M,

Zareno J,

Whitmore LA,

Mogilner A &

Horwitz AR

2008 Actin and alpha-actinin orchestrate the assembly and maturation of nascent adhesions in a myosin II motor-independent manner. Nature Cell Biology 10 1039–1050doi:10.1038/ncb1763.

CrossRef Medline Web of Science Google Scholar

[100] Choi CK,

[101] Vicente-Manzanares M,

[102] Zareno J,

[103] Whitmore LA,

[104] Mogilner A &

[105] Horwitz AR

[106] ↵

Colige A,

Sieron AL,

Li SW,

Schwarze U,

Petty E,

Wertelecki W,

Wilcox W,

Krakow D,

Cohn DH,

Reardon W

et al.

1999 Human Ehlers–Danlos syndrome type VII C and bovine dermatosparaxis are caused by mutations in the procollagen I N-proteinase gene. American Journal of Human Genetics 65 308–317doi:10.1086/302504.

CrossRef Medline Web of Science Google Scholar

[107] Colige A,

[108] Sieron AL,

[109] Li SW,

[110] Schwarze U,

[111] Petty E,

[112] Wertelecki W,

[113] Wilcox W,

[114] Krakow D,

[115] Cohn DH,

[116] Reardon W

[117] et al.

[118] ↵

Colognato H &

Yurchenco PD

2000 Form and function: the laminin family of heterotrimers. Developmental Dynamics 218 213–234doi:10.1002/(SICI)1097-0177(200006)218:2<213::AID-DVDY1>3.0.CO;2-R.

CrossRef Medline Web of Science Google Scholar

[119] Colognato H &

[120] Yurchenco PD

[121] ↵

Daoud J,

Petropavlovskaia M,

Rosenberg L &

Tabrizian M

2010 The effect of extracellular matrix components on the preservation of human islet function in vitro. Biomaterials 31 1676–1682doi:10.1016/j.biomaterials.2009.11.057.

CrossRef Medline Web of Science Google Scholar

[122] Daoud J,

[123] Petropavlovskaia M,

[124] Rosenberg L &

[125] Tabrizian M

[126] ↵

David G

1992 Structural and functional diversity of the heparan sulfate proteoglycans. Advances in Experimental Medicine and Biology 313 69–78.

CrossRef Medline Web of Science Google Scholar

[127] David G

[128] ↵

Day AJ &

Sheehan JK

2001 Hyaluronan: polysaccharide chaos to protein organisation. Current Opinion in Structural Biology 11 617–622doi:10.1016/S0959-440X(00)00256-6.

CrossRef Medline Web of Science Google Scholar

[129] Day AJ &

[130] Sheehan JK

[131] ↵

Dempsey LA,

Brunn GJ &

Platt JL

2000 Heparanase, a potential regulator of cell–matrix interactions. Trends in Biochemical Sciences 25 349–351doi:10.1016/S0968-0004(00)01619-4.

CrossRef Medline Web of Science Google Scholar

[132] Dempsey LA,

[133] Brunn GJ &

[134] Platt JL

[135] ↵

Desgrosellier JS &

Cheresh DA

2010 Integrins in cancer: biological implications and therapeutic opportunities. Nature Reviews. Cancer 10 9–22doi:10.1038/nrc2748.

CrossRef Medline Web of Science Google Scholar

[136] Desgrosellier JS &

[137] Cheresh DA

[138] ↵

Discher DE,

Mooney DJ &

Zandstra PW

2009 Growth factors, matrices, and forces combine and control stem cells. Science 324 1673–1677doi:10.1126/science.1171643.

Abstract/FREE Full Text

[139] Discher DE,

[140] Mooney DJ &

[141] Zandstra PW

[142] ↵

Drucker L,

Afensiev F,

Radnay J,

Shapira H &

Lishner M

2004 Co-administration of simvastatin and cytotoxic drugs is advantageous in myeloma cell lines. Anticancer Drugs 15 79–84doi:10.1097/00001813-200401000-00012.

CrossRef Medline Google Scholar

[143] Drucker L,

[144] Afensiev F,

[145] Radnay J,

[146] Shapira H &

[147] Lishner M

[148] ↵

Edin ML &

Juliano RL

2005 Raf-1 serine 338 phosphorylation plays a key role in adhesion-dependent activation of extracellular signal-regulated kinase by epidermal growth factor. Molecular and Cellular Biology 25 4466–4475doi:10.1128/MCB.25.11.4466-4475.2005.

Abstract/FREE Full Text

[149] Edin ML &

[150] Juliano RL

[151] ↵

Engler AJ,

Sen S,

Sweeney HL &

Discher DE

2006 Matrix elasticity directs stem cell lineage specification. Cell 126 677–689doi:10.1016/j.cell.2006.06.044.

CrossRef Medline Web of Science Google Scholar

[152] Engler AJ,

[153] Sen S,

[154] Sweeney HL &

[155] Discher DE

[156] ↵

Esko JD &

Selleck SB

2002 Order out of chaos: assembly of ligand binding sites in heparan sulfate. Annual Review of Biochemistry 71 435–471doi:10.1146/annurev.biochem.71.110601.135458.

CrossRef Medline Web of Science Google Scholar

[157] Esko JD &

[158] Selleck SB

[159] ↵

Faham S,

Hileman RE,

Fromm JR,

Linhardt RJ &

Rees DC

1996 Heparin structure and interactions with basic fibroblast growth factor. Science 271 1116–1120doi:10.1126/science.271.5252.1116.

Abstract

[160] Faham S,

[161] Hileman RE,

[162] Fromm JR,

[163] Linhardt RJ &

[164] Rees DC

[165] ↵

Friedl P &

Wolf K

2009 Proteolytic interstitial cell migration: a five-step process. Cancer Metastasis Reviews 28 129–135doi:10.1007/s10555-008-9174-3.

CrossRef Medline Web of Science Google Scholar

[166] Friedl P &

[167] Wolf K

[168] ↵

Friedl A,

Chang Z,

Tierney A &

Rapraeger AC

1997 Differential binding of fibroblast growth factor-2 and -7 to basement membrane heparan sulfate: comparison of normal and abnormal human tissues. American Journal of Pathology 150 1443–1455.

Medline Web of Science Google Scholar

[169] Friedl A,

[170] Chang Z,

[171] Tierney A &

[172] Rapraeger AC

[173] ↵

Friedl A,

Filla M &

Rapraeger AC

2001 Tissue-specific binding by FGF and FGF receptors to endogenous heparan sulfates. Methods in Molecular Biology 171 535–546doi:10.1385/1-59259-209-0:535.

Medline Google Scholar

[174] Friedl A,

[175] Filla M &

[176] Rapraeger AC

[177] ↵

Galbraith CG,

Yamada KM &

Sheetz MP

2002 The relationship between force and focal complex development. Journal of Cell Biology 159 695–705doi:10.1083/jcb.200204153.

Abstract/FREE Full Text

[178] Galbraith CG,

[179] Yamada KM &

[180] Sheetz MP

[181] ↵

Gao Y,

Xiao Q,

Ma H,

Li L,

Liu J,

Feng Y,

Fang Z,

Wu J,

Han X,

Zhang J

et al.

2010 LKB1 inhibits lung cancer progression through lysyl oxidase and extracellular matrix remodeling. PNAS 107 18892–18897doi:10.1073/pnas.1004952107.

Abstract/FREE Full Text

[182] Gao Y,

[183] Xiao Q,

[184] Ma H,

[185] Li L,

[186] Liu J,

[187] Feng Y,

[188] Fang Z,

[189] Wu J,

[190] Han X,

[191] Zhang J

[192] et al.

[193] ↵

Garcia AJ,

Coffinier C,

Larrain J,

Oelgeschlager M &

De Robertis EM

2002 Chordin-like CR domains and the regulation of evolutionarily conserved extracellular signaling systems. Gene 287 39–47doi:10.1016/S0378-1119(01)00827-7.

CrossRef Medline Web of Science Google Scholar

[194] Garcia AJ,

[195] Coffinier C,

[196] Larrain J,

[197] Oelgeschlager M &

[198] De Robertis EM

[199] ↵

Geiger B,

Bershadsky A,

Pankov R &

Yamada KM

2001 Transmembrane crosstalk between the extracellular matrix–cytoskeleton crosstalk. Nature Reviews. Molecular Cell Biology 2 793–805doi:10.1038/35099066.

CrossRef Medline Web of Science Google Scholar

[200] Geiger B,

[201] Bershadsky A,

[202] Pankov R &

[203] Yamada KM

[204] ↵

Geiger B,

Spatz JP &

Bershadsky AD

2009 Environmental sensing through focal adhesions. Nature Reviews. Molecular Cell Biology 10 21–33doi:10.1038/nrm2593.

CrossRef Medline Web of Science Google Scholar

[205] Geiger B,

[206] Spatz JP &

[207] Bershadsky AD

[208] ↵

Goel HL,

Breen M,

Zhang J,

Das I,

Aznavoorian-Cheshire S,

Greenberg NM,

Elgavish A &

Languino LR

2005 beta1A integrin expression is required for type 1 insulin-like growth factor receptor mitogenic and transforming activities and localization to focal contacts. Cancer Research 65 6692–6700doi:10.1158/0008-5472.CAN-04-4315.

Abstract/FREE Full Text

[209] Goel HL,

[210] Breen M,

[211] Zhang J,

[212] Das I,

[213] Aznavoorian-Cheshire S,

[214] Greenberg NM,

[215] Elgavish A &

[216] Languino LR

[217] ↵

Grobe K &

Esko JD

2002 Regulated translation of heparan sulfate N-acetylglucosamine N-deacetylase/n-sulfotransferase isozymes by structured 5′-untranslated regions and internal ribosome entry sites. Journal of Biological Chemistry 277 30699–30706doi:10.1074/jbc.M111904200.

Abstract/FREE Full Text

[218] Grobe K &

[219] Esko JD

[220] ↵

Guimond SE &

Turnbull JE

1999 Fibroblast growth factor receptor signalling is dictated by specific heparan sulphate saccharides. Current Biology 9 1343–1346doi:10.1016/S0960-9822(00)80060-3.

CrossRef Medline Web of Science Google Scholar

[221] Guimond SE &

[222] Turnbull JE

[223] ↵

Guimond SE,

Turnbull JE &

Yates EA

2006 Engineered bio-active polysaccharides from heparin. Macromolecular Bioscience 6 681–686doi:10.1002/mabi.200600042.

CrossRef Medline Web of Science Google Scholar

[224] Guimond SE,

[225] Turnbull JE &

[226] Yates EA

[227] ↵

Guimond SE,

Rudd TR,

Skidmore MA,

Ori A,

Gaudesi D,

Cosentino C,

Guerrini M,

Edge R,

Collison D,

McInnes E

et al.

2009 Cations modulate polysaccharide structure to determine FGF–FGFR signaling: a comparison of signaling and inhibitory polysaccharide interactions with FGF-1 in solution. Biochemistry 48 4772–4779doi:10.1021/bi802318z.

CrossRef Medline Web of Science Google Scholar

[228] Guimond SE,

[229] Rudd TR,

[230] Skidmore MA,

[231] Ori A,

[232] Gaudesi D,

[233] Cosentino C,

[234] Guerrini M,

[235] Edge R,

[236] Collison D,

[237] McInnes E

[238] et al.

[239] ↵

Hanks SK,

Calalb MB,

Harper MC &

Patel SK

1992 Focal adhesion protein-tyrosine kinase phosphorylated in response to cell attachment to fibronectin. PNAS 89 8487–8491doi:10.1073/pnas.89.18.8487.

Abstract/FREE Full Text

[240] Hanks SK,

[241] Calalb MB,

[242] Harper MC &

[243] Patel SK

[244] ↵

Hanna E,

Quick J &

Libutti SK

2009 The tumour microenvironment: a novel target for cancer therapy. Oral Disease 15 8–17doi:10.1111/j.1601-0825.2008.01471.x.

CrossRef Google Scholar

[245] Hanna E,

[246] Quick J &

[247] Libutti SK

[248] ↵

Hardingham TE &

Fosang AJ

1992 Proteoglycans: many forms and many functions. FASEB Journal 6 861–870.

Abstract

[249] Hardingham TE &

[250] Fosang AJ

[251] ↵

Hemler ME &

Lobb RR

1995 The leukocyte beta 1 integrins. Current Opinion in Hematology 2 61–67doi:10.1097/00062752-199502010-00009.

CrossRef Medline Google Scholar

[252] Hemler ME &

[253] Lobb RR

[254] ↵

Hildebrand A,

Romaris M,

Rasmussen LM,

Heinegard D,

Twardzik DR,

Border WA &

Ruoslahti E

1994 Interaction of the small interstitial proteoglycans biglycan, decorin and fibromodulin with transforming growth factor beta. Biochemical Journal 302 527–534.

Abstract/FREE Full Text

[255] Hildebrand A,

[256] Romaris M,

[257] Rasmussen LM,

[258] Heinegard D,

[259] Twardzik DR,

[260] Border WA &

[261] Ruoslahti E

[262] ↵

Hu Y,

Guimond SE,

Travers P,

Cadman SM,

Hohenester E,

Turnbull JE,

Kim SH &

Bouloux PMG

2009 Novel mechanisms of fibroblast growth factor receptor 1 regulation by extracellular matrix protein anosmin-1. Journal of Biological Chemistry 284 29905–29920doi:10.1074/jbc.M109.049155.

Abstract/FREE Full Text

[263] Hu Y,

[264] Guimond SE,

[265] Travers P,

[266] Cadman SM,

[267] Hohenester E,

[268] Turnbull JE,

[269] Kim SH &

[270] Bouloux PMG

[271] ↵

Hulett MD,

Freeman C,

Hamdorf BJ,

Baker RT,

Harris MJ &

Parish CR

1999 Cloning of mammalian heparanase, an important enzyme in tumor invasion and metastasis. Nature Medicine 5 803–809doi:10.1038/10525.

CrossRef Medline Web of Science Google Scholar

[272] Hulett MD,

[273] Freeman C,

[274] Hamdorf BJ,

[275] Baker RT,

[276] Harris MJ &

[277] Parish CR

[278] ↵

Hulmes DJ

2002 Building collagen molecules, fibrils, and suprafibrillar structures. Journal of Structural Biology 137 2–10doi:10.1006/jsbi.2002.4450.

CrossRef Medline Web of Science Google Scholar

[279] Hulmes DJ

[280] ↵

Humphries JD,

Wang P,

Streuli C,

Geiger B,

Humphries MJ &

Ballestrem C

2007 Vinculin controls focal adhesion formation by direct interactions with talin and actin. Journal of Cell Biology 179 1043–1057doi:10.1083/jcb.200703036.

Abstract/FREE Full Text

[281] Humphries JD,

[282] Wang P,

[283] Streuli C,

[284] Geiger B,

[285] Humphries MJ &

[286] Ballestrem C

[287] ↵

Ingber DE,

Madri JA &

Jamieson JD

1981 Role of basal lamina in neoplastic disorganization of tissue architecture. PNAS 78 3901–3905doi:10.1073/pnas.78.6.3901.

Abstract/FREE Full Text

[288] Ingber DE,

[289] Madri JA &

[290] Jamieson JD

[291] ↵

Jaffe AB &

Hall A

2005 Rho GTPases: biochemistry and biology. Annual Review of Cell and Development Biology 21 247–269doi:10.1146/annurev.cellbio.21.020604.150721.

CrossRef Google Scholar

[292] Jaffe AB &

[293] Hall A

[294] ↵

Jiang F,

Horber H,

Howard J &

Muller DJ

2004 Assembly of collagen into microribbons: effects of pH and electrolytes. Journal of Structural Biology 148 268–278doi:10.1016/j.jsb.2004.07.001.

CrossRef Medline Web of Science Google Scholar

[295] Jiang F,

[296] Horber H,

[297] Howard J &

[298] Muller DJ

[299] ↵

Kakkad SM,

Solaiyappan M,

O'Rourke B,

Stasinopoulos I,

Ackerstaff E,

Raman V,

Bhujwalla ZM &

Glunde K

2010 Hypoxic tumor microenvironments reduce collagen I fiber density. Neoplasia 12 608–617.

Medline Web of Science Google Scholar

[300] Kakkad SM,

[301] Solaiyappan M,

[302] O'Rourke B,

[303] Stasinopoulos I,

[304] Ackerstaff E,

[305] Raman V,

[306] Bhujwalla ZM &

[307] Glunde K

[308] ↵

Kalluri R

2003 Basement membranes: structure, assembly and role in tumour angiogenesis. Nature Reviews. Cancer 3 422–433doi:10.1038/nrc1094.

CrossRef Medline Web of Science Google Scholar

[309] Kalluri R

[310] ↵

Kalluri R &

Zeisberg M

2006 Fibroblasts in cancer. Nature Reviews. Cancer 6 392–401doi:10.1038/nrc1877.

CrossRef Medline Web of Science Google Scholar

[311] Kalluri R &

[312] Zeisberg M

[313] ↵

Kamei N,

Kwon SM,

Alev C,

Ishikawa M,

Yokoyama A,

Nakanishi K,

Yamada K,

Horii M,

Nishimura H,

Takaki S

et al.

2010 Lnk deletion reinforces the function of bone marrow progenitors in promoting neovascularization and astrogliosis following spinal cord injury. Stem Cells 28 365–375doi:10.1002/stem.243.

Medline Web of Science Google Scholar

[314] Kamei N,

[315] Kwon SM,

[316] Alev C,

[317] Ishikawa M,

[318] Yokoyama A,

[319] Nakanishi K,

[320] Yamada K,

[321] Horii M,

[322] Nishimura H,

[323] Takaki S

[324] et al.

[325] ↵

Kan M,

Wang F,

Xu J,

Crabb JW,

Hou J &

McKeehan WL

1993 An essential heparin-binding domain in the fibroblast growth factor receptor kinase. Science 259 1918–1921doi:10.1126/science.8456318.

Abstract/FREE Full Text

[326] Kan M,

[327] Wang F,

[328] Xu J,

[329] Crabb JW,

[330] Hou J &

[331] McKeehan WL

[332] ↵

Kenny PA &

Bissell MJ

2003 Tumor reversion: correction of malignant behavior by microenvironmental cues. International Journal of Cancer 107 688–695doi:10.1002/ijc.11491.

CrossRef Medline Web of Science Google Scholar

[333] Kenny PA &

[334] Bissell MJ

[335] ↵

Kielty CM,

Sherratt MJ &

Shuttleworth CA

2002 Elastic fibres. Journal of Cell Science 115 2817–2828.

Abstract/FREE Full Text

[336] Kielty CM,

[337] Sherratt MJ &

[338] Shuttleworth CA

[339] ↵

Kim SH &

Kim SH

2008 Antagonistic effect of EGF on FAK phosphorylation/dephosphorylation in a cell. Cell Biochemistry and Function 26 539–547doi:10.1002/cbf.1457.

CrossRef Medline Web of Science Google Scholar

[340] Kim SH &

[341] Kim SH

[342] ↵

Kirkpatrick CA,

Dimitroff BD,

Rawson JM &

Selleck SB

2004 Spatial regulation of Wingless morphogen distribution and signaling by Dally-like protein. Developmental Cell 7 513–523doi:10.1016/j.devcel.2004.08.004.

CrossRef Medline Web of Science Google Scholar

[343] Kirkpatrick CA,

[344] Dimitroff BD,

[345] Rawson JM &

[346] Selleck SB

[347] ↵

Kiselyov VV,

Skladchikova G,

Hinsby AM,

Jensen PH,

Kulahin N,

Soroka V,

Pedersen N,

Tsetlin V,

Poulsen FM,

Berezin V

et al.

2003 Structural basis for a direct interaction between FGFR1 and NCAM and evidence for a regulatory role of ATP. Structure 11 691–701doi:10.1016/S0969-2126(03)00096-0.

CrossRef Medline Google Scholar

[348] Kiselyov VV,

[349] Skladchikova G,

[350] Hinsby AM,

[351] Jensen PH,

[352] Kulahin N,

[353] Soroka V,

[354] Pedersen N,

[355] Tsetlin V,

[356] Poulsen FM,

[357] Berezin V

[358] et al.

[359] ↵

Kjellen L &

Lindahl U

1991 Proteoglycans: structures and interactions. Annual Review of Biochemistry 60 443–475doi:10.1146/annurev.bi.60.070191.002303.

CrossRef Medline Web of Science Google Scholar

[360] Kjellen L &

[361] Lindahl U

[362] ↵

Knecht M

1988 Plasminogen activator is associated with the extracellular matrix of ovarian granulosa cells. Molecular and Cellular Endocrinology 56 1–9doi:10.1016/0303-7207(88)90002-0.

CrossRef Medline Web of Science Google Scholar

[363] Knecht M

[364] ↵

Kresse H &

Schonherr E

2001 Proteoglycans of the extracellular matrix and growth control. Journal of Cellular Physiology 189 266–274doi:10.1002/jcp.10030.

CrossRef Medline Web of Science Google Scholar

[365] Kresse H &

[366] Schonherr E

[367] ↵

Kreuger J,

Perez L,

Giraldez AJ &

Cohen SM

2004 Opposing activities of Dally-like glypican at high and low levels of Wingless morphogen activity. Developmental Cell 7 503–512doi:10.1016/j.devcel.2004.08.005.

CrossRef Medline Web of Science Google Scholar

[368] Kreuger J,

[369] Perez L,

[370] Giraldez AJ &

[371] Cohen SM

[372] ↵

van Kuppevelt TH,

Dennissen MA,

van Venrooij WJ,

Hoet RM &

Veerkamp JH

1998 Generation and application of type-specific anti-heparan sulfate antibodies using phage display technology. Further evidence for heparan sulfate heterogeneity in the kidney. Journal of Biological Chemistry 273 12960–12966doi:10.1074/jbc.273.21.12960.

Abstract/FREE Full Text

[373] van Kuppevelt TH,

[374] Dennissen MA,

[375] van Venrooij WJ,

[376] Hoet RM &

[377] Veerkamp JH

[378] ↵

Lamanna WC,

Baldwin RJ,

Padva M,

Kalus I,

Ten DG,

van Kuppevelt TH,

Gallagher JT,

von FK,

Dierks T &

Merry CL

2006 Heparan sulfate 6-O-endosulfatases: discrete in vivo activities and functional co-operativity. Biochemical Journal 400 63–73doi:10.1042/BJ20060848.

Abstract/FREE Full Text

[379] Lamanna WC,

[380] Baldwin RJ,

[381] Padva M,

[382] Kalus I,

[383] Ten DG,

[384] van Kuppevelt TH,

[385] Gallagher JT,

[386] von FK,

[387] Dierks T &

[388] Merry CL

[389] ↵

Legate KR,

Wickstrom SA &

Fassler R

2009 Genetic and cell biological analysis of integrin outside-in signaling. Genes and Development 23 397–418doi:10.1101/gad.1758709.

Abstract/FREE Full Text

[390] Legate KR,

[391] Wickstrom SA &

[392] Fassler R

[393] ↵

Li JP &

Vlodavsky I

2009 Heparin, heparan sulfate and heparanase in inflammatory reactions. Thrombosis and Haemostasis 102 823–828doi:10.1160/TH09-02-0091.

Medline Web of Science Google Scholar

[394] Li JP &

[395] Vlodavsky I

[396] ↵

Lindahl U,

Kusche M,

Lidholt K &

Oscarsson LG

1989 Biosynthesis of heparin and heparan sulfate. Annals of the New York Academy of Sciences 556 36–50doi:10.1111/j.1749-6632.1989.tb22488.x.

CrossRef Medline Web of Science Google Scholar

[397] Lindahl U,

[398] Kusche M,

[399] Lidholt K &

[400] Oscarsson LG

[401] ↵

Lock R &

Debnath J

2008 Extracellular matrix regulation of autophagy. Current Opinion in Cell Biology 20 583–588doi:10.1016/j.ceb.2008.05.002.

CrossRef Medline Web of Science Google Scholar

[402] Lock R &

[403] Debnath J

[404] ↵

Maffini MV,

Soto AM,

Calabro JM,

Ucci AA &

Sonnenschein C

2004 The stroma as a crucial target in rat mammary gland carcinogenesis. Journal of Cell Science 117 1495–1502doi:10.1242/jcs.01000.

Abstract/FREE Full Text

[405] Maffini MV,

[406] Soto AM,

[407] Calabro JM,

[408] Ucci AA &

[409] Sonnenschein C

[410] ↵

Maffini MV,

Calabro JM,

Soto AM &

Sonnenschein C

2005 Stromal regulation of neoplastic development: age-dependent normalization of neoplastic mammary cells by mammary stroma. American Journal of Pathology 167 1405–1410doi:10.1016/S0002-9440(10)61227-8.

CrossRef Medline Web of Science Google Scholar

[411] Maffini MV,

[412] Calabro JM,

[413] Soto AM &

[414] Sonnenschein C

[415] ↵

Manon-Jensen T,

Itoh Y &

Couchman JR

2010 Proteoglycans in health and disease: the multiple roles of syndecan shedding. FEBS Journal 277 3876–3889doi:10.1111/j.1742-4658.2010.07798.x.

CrossRef Medline Web of Science Google Scholar

[416] Manon-Jensen T,

[417] Itoh Y &

[418] Couchman JR

[419] ↵

Marastoni S,

Ligresti G,

Lorenzon E,

Colombatti A &

Mongiat M

2008 Extracellular matrix: a matter of life and death. Connective Tissue Research 49 203–206doi:10.1080/03008200802143190.

CrossRef Medline Web of Science Google Scholar

[420] Marastoni S,

[421] Ligresti G,

[422] Lorenzon E,

[423] Colombatti A &

[424] Mongiat M

[425] ↵

Mitra SK,

Hanson DA &

Schlaepfer DD

2005 Focal adhesion kinase: in command and control of cell motility. Nature Reviews. Molecular Cell Biology 6 56–68doi:10.1038/nrm1549.

CrossRef Medline Web of Science Google Scholar

[426] Mitra SK,

[427] Hanson DA &

[428] Schlaepfer DD

[429] ↵

Moser M,

Nieswandt B,

Ussar S,

Pozgajova M &

Fassler R

2008 Kindlin-3 is essential for integrin activation and platelet aggregation. Nature Medicine 14 325–330doi:10.1038/nm1722.

CrossRef Medline Web of Science Google Scholar

[430] Moser M,

[431] Nieswandt B,

[432] Ussar S,

[433] Pozgajova M &

[434] Fassler R

[435] ↵

Mott JD &

Werb Z

2004 Regulation of matrix biology by matrix metalloproteinases. Current Opinion in Cell Biology 16 558–564doi:10.1016/j.ceb.2004.07.010.

CrossRef Medline Web of Science Google Scholar

[436] Mott JD &

[437] Werb Z

[438] ↵

Mundhenke C,

Meyer K,

Drew S &

Friedl A

2002 Heparan sulfate proteoglycans as regulators of fibroblast growth factor-2 receptor binding in breast carcinomas. American Journal of Pathology 160 185–194doi:10.1016/S0002-9440(10)64362-3.

CrossRef Medline Web of Science Google Scholar

[439] Mundhenke C,

[440] Meyer K,

[441] Drew S &

[442] Friedl A

[443] ↵

Nagai N,

Habuchi H,

Esko JD &

Kimata K

2004 Stem domains of heparan sulfate 6-O-sulfotransferase are required for Golgi localization, oligomer formation and enzyme activity. Journal of Cell Science 117 3331–3341doi:10.1242/jcs.01191.

Abstract/FREE Full Text

[444] Nagai N,

[445] Habuchi H,

[446] Esko JD &

[447] Kimata K

[448] ↵

Narita K,

Staub J,

Chien J,

Meyer K,

Bauer M,

Friedl A,

Ramakrishnan S &

Shridhar V

2006 HSulf-1 inhibits angiogenesis and tumorigenesis in vivo. Cancer Research 66 6025–6032doi:10.1158/0008-5472.CAN-05-3582.

Abstract/FREE Full Text

[449] Narita K,

[450] Staub J,

[451] Chien J,

[452] Meyer K,

[453] Bauer M,

[454] Friedl A,

[455] Ramakrishnan S &

[456] Shridhar V

[457] ↵

Ori A,

Free P,

Courty J,

Wilkinson MC &

Fernig DG

2009 Identification of heparin-binding sites in proteins by selective labeling. Molecular and Cellular Proteomics 8 2256–2265doi:10.1074/mcp.M900031-MCP200.

CrossRef Google Scholar

[458] Ori A,

[459] Free P,

[460] Courty J,

[461] Wilkinson MC &

[462] Fernig DG

[463] ↵

Ornitz DM,

Xu J,

Colvin JS,

McEwen DG,

MacArthur CA,

Coulier F,

Gao G &

Goldfarb M

1996 Receptor specificity of the fibroblast growth factor family. Journal of Biological Chemistry 271 15292–15297doi:10.1074/jbc.271.25.15292.

Abstract/FREE Full Text

[464] Ornitz DM,

[465] Xu J,

[466] Colvin JS,

[467] McEwen DG,

[468] MacArthur CA,

[469] Coulier F,

[470] Gao G &

[471] Goldfarb M

[472] ↵

Overall CM &

Lopez-Otin C

2002 Strategies for MMP inhibition in cancer: innovations for the post-trial era. Nature Reviews. Cancer 2 657–672doi:10.1038/nrc884.

CrossRef Medline Web of Science Google Scholar

[473] Overall CM &

[474] Lopez-Otin C

[475] ↵

Park JH,

Ryu JM &

Han HJ

2011 Involvement of caveolin-1 in fibronectin-induced mouse embryonic stem cell proliferation: role of FAK, RhoA, PI3K/Akt, and ERK 1/2 pathways. Journal of Cellular Physiology 226 267–275doi:10.1002/jcp.22338.

CrossRef Medline Web of Science Google Scholar

[476] Park JH,

[477] Ryu JM &

[478] Han HJ

[479] ↵

Patel VN,

Knox SM,

Likar KM,

Lathrop CA,

Hossain R,

Eftekhari S,

Whitelock JM,

Elkin M,

Vlodavsky I &

Hoffman MP

2007 Heparanase cleavage of perlecan heparan sulfate modulates FGF10 activity during ex vivo submandibular gland branching morphogenesis. Development 134 4177–4186doi:10.1242/dev.011171.

Abstract/FREE Full Text

[480] Patel VN,

[481] Knox SM,

[482] Likar KM,

[483] Lathrop CA,

[484] Hossain R,

[485] Eftekhari S,

[486] Whitelock JM,

[487] Elkin M,

[488] Vlodavsky I &

[489] Hoffman MP

[490] ↵

Pelham RJ Jr. &

Wang Y

1997 Cell locomotion and focal adhesions are regulated by substrate flexibility. PNAS 94 13661–13665doi:10.1073/pnas.94.25.13661.

Abstract/FREE Full Text

[491] Pelham RJ Jr. &

[492] Wang Y

[493] ↵

Pinhal MA,

Smith B,

Olson S,

Aikawa J,

Kimata K &

Esko JD

2001 Enzyme interactions in heparan sulfate biosynthesis: uronosyl 5-epimerase and 2-O-sulfotransferase interact in vivo. PNAS 98 12984–12989doi:10.1073/pnas.241175798.

Abstract/FREE Full Text

[494] Pinhal MA,

[495] Smith B,

[496] Olson S,

[497] Aikawa J,

[498] Kimata K &

[499] Esko JD

[500] ↵

del Pozo MA,

Alderson NB,

Kiosses WB,

Chiang HH,

Anderson RG &

Schwartz MA

2004 Integrins regulate Rac targeting by internalization of membrane domains. Science 303 839–842doi:10.1126/science.1092571.

Abstract/FREE Full Text

[501] del Pozo MA,

Journal of Endocrinology

Extracellular matrix and cell signalling: the dynamic cooperation of integrin, proteoglycan and growth factor receptor

Abstract

Extracellular matrix as structural support and binding platform

Features of the physical adhesion surface and cell signalling

Integrins, the inside-out and outside-in signalling

Diverse molecular interactions at the adhesion sites

Src–FAK: the focal point for integrin signalling

ECM as the organising centre for growth factor receptor signal regulation

Integrin and growth factor receptor signalling

Role of proteoglycans in signal regulation

Role of HSPG in FGF and VEGF signalling

ECM proteases and heparanase

Matrix metalloproteinases

A disintegrin and metalloproteinase with thrombospondin motif

Heparanase

Role of ECM in endocrine disease and cancer

ECM and the endocrine system

ECM as tumour microenvironment

HSPG in disease mechanisms

Implications for future research and ECM as a therapeutic target

Declaration of interest

Funding

References

This Article

Article Metrics

Services

Citing Articles

Google Scholar

PubMed

Related Content

Social Bookmarking

Navigate This Article

Current Issue

Most

Viewed

Cited