Download
1 / 73
730 likes | 1.17k Views
Chapter 15 The extracellular matrix and cell adhesion By George Plopper 15.1 Introduction Cell-cell junctions are specialized protein complexes that allow neighboring cells to: adhere to one another communicate with one another The extracellular matrix is a dense network of proteins that:
E N D
Chapter 15 The extracellular matrix and cell adhesion By George Plopper
15.1 Introduction • Cell-cell junctions are specialized protein complexes that allow neighboring cells to: • adhere to one another • communicate with one another • The extracellular matrix is a dense network of proteins that: • lies between cells • is made by the cells within the network
15.1 Introduction • Cells express receptors for extracellular matrix proteins. • The proteins in the extracellular matrix and cell junctions control: • the three-dimensional organization of cells in tissues • the growth, movement, shape, and differentiation of these cells
15.2 A brief history of research on the extracellular matrix • The study of the extracellular matrix and cell junctions has occurred in four historical stages. • Each is defined by the technological advances that allowed increasingly detailed examination of these structures. • Current research in this field is focused on determining how the proteins in the extracellular matrix and cell junctions control cell behavior.
15.3 Collagen provides structural support to tissues • The principal function of collagens is to provide structural support to tissues. • Collagens are a family of over 20 different extracellular matrix proteins. • Together they are the most abundant proteins in the animal kingdom.
15.3 Collagen provides structural support to tissues • All collagens are organized into triple helical, coiled-coil “collagen subunits.” • They are composed of three separate collagen polypeptides. • Collagen subunits are: • secreted from cells • then assembled into larger fibrils and fibers in the extracellular space
15.3 Collagen provides structural support to tissues • Mutations of collagen genes can lead to a wide range of diseases, from mild wrinkling to brittle bones to fatal blistering of the skin.
15.4 Fibronectins connect cells to collagenous matrices • The principal function of the extracellular matrix protein fibronectin is to connect cells to matrices that contain fibrillar collagen. • At least 20 different forms of fibronectin have been identified. • All of them arise from alternative splicing of a single fibronectin gene.
15.4 Fibronectins connect cells to collagenous matrices • The soluble forms of fibronectin are found in tissue fluids. • The insoluble forms are organized into fibers in the extracellular matrix.
15.4 Fibronectins connect cells to collagenous matrices • Fibronectin fibers consist of crosslinked polymers of fibronectin homodimers. • Fibronectin proteins contain six structural regions. • Each has a series of repeating units.
15.4 Fibronectins connect cells to collagenous matrices • Fibrin, heparan sulfate proteoglycan, and collagen: • bind to distinct regions in fibronectin • integrate fibronectin fibers into the extracellular matrix network • Some cells express integrin receptors that bind to the Arg-Gly-Asp (RGD) sequence of fibronectin.
15.5 Elastic fibers impart flexibility to tissues • The principal function of elastin is to impart elasticity to tissues. • Elastin monomers (known as tropoelastin subunits) are organized into fibers. • The fibers are so strong and stable they can last a lifetime.
15.5 Elastic fibers impart flexibility to tissues • The strength of elastic fibers arises from covalent crosslinks formed between lysine side chains in adjacent elastin monomers. • The elasticity of elastic fibers arises from the hydrophobic regions, which: • are stretched out by tensile forces • spontaneously reaggregate when the force is released
15.5 Elastic fibers impart flexibility to tissues • Assembly of tropoelastin into fibers: • occurs in the extracellular space • is controlled by a threestep process • Mutations in elastin give rise to a variety of disorders, ranging from mild skin wrinkling to death in early childhood.
15.6 Laminins provide an adhesive substrate for cells • Laminins are a family of extracellular matrix proteins. • They are found in virtually all tissues of vertebrate and invertebrate animals. • The principal functions of laminins are: • to provide an adhesive substrate for cells • to resist tensile forces in tissues
15.6 Laminins provide an adhesive substrate for cells • Laminins are heterotrimers comprising three different subunits wrapped together in a coiled-coil configuration. • Laminin heterotrimers do not form fibers. • They bind to linker proteins that enable them to form complex webs in the extracellular matrix.
15.6 Laminins provide an adhesive substrate for cells • A large number of proteins bind to laminins, including more than 20 different cell surface receptors.
15.7 Vitronectin facilitates targeted cell adhesion during blood clotting • Vitronectin is an extracellular matrix protein. • It circulates in blood plasma in its soluble form. • Vitronectin can bind to many different types of proteins, such as: • collagens • integrins • clotting factors • cell lysis factors • extracellular proteases
15.7 Vitronectin facilitates targeted cell adhesion during blood clotting • Vitronectin facilitates blood clot formation in damaged tissues. • In order to target deposition of clotting factors in tissues, vitronectin must convert from the soluble form to the insoluble form, which binds clotting factors.
15.8 Proteoglycans provide hydration to tissues • Proteoglycans consist of a central protein “core” to which long, linear chains of disaccharides, called glycosaminoglycans (GAGs), are attached. • GAG chains on proteoglycans are negatively charged. • This gives the proteoglycans a rodlike, bristly shape due to charge repulsion.
15.8 Proteoglycans provide hydration to tissues • The GAG bristles act as filters to limit the diffusion of viruses and bacteria in tissues. • Proteoglycans attract water to form gels that: • keep cells hydrated • cushion tissues against hydrostatic pressure
15.8 Proteoglycans provide hydration to tissues • Proteoglycans can bind to a variety of extracellular matrix components, including: • growth factors • structural proteins • cell surface receptors • Expression of proteoglycans is: • cell type specific • developmentally regulated
15.9 Hyaluronan is a glycosaminoglycan enriched in connective tissues • Hyaluronan is a glycosaminoglycan. • It forms enormous complexes with proteoglycans in the extracellular matrix. • These complexes are especially abundant in cartilage. • There, hyaluronan is associated with the proteoglycan aggrecan, via a linker protein.
15.9 Hyaluronan is a glycosaminoglycan enriched in connective tissues • Hyaluronan is highly negatively charged. • It binds to cations and water in the extracellular space. • This increases the stiffness of the extracellular matrix . • This provides a water cushion between cells that absorbs compressive forces. • Hyaluronan consists of repeating disaccharides linked into long chains.
15.9 Hyaluronan is a glycosaminoglycan enriched in connective tissues • Unlike other glycosaminoglycans, hyaluronans chains are: • synthesized on the cytosolic surface of the plasma membrane • translocated out of the cell • Cells bind to hyaluronan via a family of receptors known as hyladherins. • Hyladherins initiate signaling pathways that control: • cell migration • assembly of the cytoskeleton
15.10 Heparan sulfate proteoglycans are cell surface coreceptors • Heparan sulfate proteoglycans are a subset of proteoglycans. • They contain chains of the glycosaminoglycan heparan sulfate. • Most heparan sulfate is found on two families of membrane-bound proteoglycans: • the syndecans • the glypicans
15.10 Heparan sulfate proteoglycans are cell surface coreceptors • Heparan sulfates are composed of distinct combinations of more than 30 different sugar subunits. • This allows for great variety in heparan sulfate proteoglycan structure and function. • Cell surface heparan sulfate proteoglycans: • are expressed on many types of cells • bind to over 70 different proteins
15.10 Heparan sulfate proteoglycans are cell surface coreceptors • Cell surface heparan sulfate proteoglycans • assist in the internalization of some proteins • act as coreceptors for: • soluble proteins such as growth factors • insoluble proteins such as extracellular matrix proteins • Genetic studies in fruit flies show that heparan sulfate proteoglycans function in: • growth factor signaling • development
15.11 The basal lamina is a specialized extracellular matrix • The basal lamina is a thin sheet of extracellular matrix • is composed of at least two distinct layers • is found at: • the basal surface of epithelial sheets • neuromuscular junctions
15.11 The basal lamina is a specialized extracellular matrix • The basement membrane consists of the basal lamina connected to a network of collagen fibers. • The basal lamina functions as: • a supportive network to maintain epithelial tissues • a diffusion barrier • a collection site for soluble proteins such as growth factors • a guidance signal for migrating neurons
15.11 The basal lamina is a specialized extracellular matrix • The components of the basal lamina vary in different tissue types. • But most share four principal extracellular matrix components: • sheets of collagen IV and laminin are held together by: • heparan sulfate proteoglycans • the linker protein nidogen
15.12 Proteases degrade extracellular matrix components • Cells must routinely degrade and replace their extracellular matrix as a normal part of • development • wound healing
15.12 Proteases degrade extracellular matrix components • Extracellular matrix proteins are degraded by specific proteases, which cells secrete in an inactive form. • These proteases are only activated in the tissues where they are needed. • Activation usually occurs by proteolytic cleavage of a propeptide on the protease.
15.12 Proteases degrade extracellular matrix components • The matrix metalloproteinase (MMP) family is one of the most abundant classes of these proteases. • It can degrade all of the major classes of extracellular matrix proteins. • MMPs can activate one another by cleaving off their propeptides. • This results in a cascade-like effect of protease activation that can lead to rapid degradation of extracellular matrix proteins.
15.12 Proteases degrade extracellular matrix components • ADAMs are a second class of proteases that degrade the extracellular matrix. • These proteases also bind to integrin extracellular matrix receptors. • Thus, they help regulate extracellular matrix assembly and degradation.
15.12 Proteases degrade extracellular matrix components • Cells secrete inhibitors of these proteases to protect themselves from unnecessary degradation. • Mutations in the matrix metalloproteinase-2 gene give rise to numerous skeletal abnormalities in humans. • This reflects the importance of extracellular matrix remodeling during development.
15.13 Most integrins are receptors for extracellular matrix proteins • Virtually all animal cells express integrins. • They are the most abundant and widely expressed class of extracellular matrix protein receptors. • Some integrins associate with other transmembrane proteins.
15.13 Most integrins are receptors for extracellular matrix proteins • Integrins are composed of two distinct subunits, known as α and βchains. • The extracellular portions of both chains bind to extracellular matrix proteins • The cytoplasmic portions bind to cytoskeletal and signaling proteins.
15.13 Most integrins are receptors for extracellular matrix proteins • In vertebrates, there are many αand βintegrin subunits. • These combine to form at least 24 different αβheterodimeric receptors. • Most cells express more than one type of integrin receptor. • The types of receptor expressed by a cell can change: • over time or • in response to different environmental conditions
15.13 Most integrins are receptors for extracellular matrix proteins • Integrin receptors bind to specific amino acid sequences in a variety of extracellular matrix proteins. • All of the known sequences contain at least one acidic amino acid.
15.14 Integrin receptors participate in cell signaling • Integrins are signaling receptors that control both: • cell binding to extracellular matrix proteins • intracellular responses following adhesion • Integrins have no enzymatic activity of their own. • Instead, they interact with adaptor proteins that link them to signaling proteins.
15.14 Integrin receptors participate in cell signaling • Two processes regulate the strength of integrin binding to extracellular matrix proteins: • affinity modulation • varying the binding strength of individual receptors • avidity modulation • varying the clustering of receptors
15.14 Integrin receptors participate in cell signaling • Changes in integrin receptor conformation are central to both types of modulation. • They can result from changes: • at the cytoplasmic tails of the receptor subunits or • in the concentration of extracellular cations
15.14 Integrin receptors participate in cell signaling • In inside-out signaling, changes in receptor conformation result from intracellular signals that originate elsewhere in the cell. • For example, at another receptor • In outside-in signaling, signals initiated at a receptor are propagated to other parts of the cell. • For example, upon ligand binding
15.14 Integrin receptors participate in cell signaling • The cytoplasmic proteins associated with integrin clusters vary greatly depending on: • the types of integrins and extracellular matrix proteins engaged. • The resulting cellular responses to integrin outside-in signaling vary accordingly. • Many of the integrin signaling pathways overlap with growth factor receptor pathways.
15.15 Integrins and extracellular matrix molecules play key roles in development • Gene knockout by homologous recombination has been applied in mice to; • over 40 different extracellular matrix proteins • 21 integrin genes • Some genetic knockouts are lethal, while others have mild phenotypes.
15.15 Integrins and extracellular matrix molecules play key roles in development • Targeted disruption of the β1 integrin gene has revealed that it plays a critical role in: • the organization of the skin • red blood cell development
15.16 Tight junctions form selectively permeable barriers between cells • Tight junctions are part of the junctional complex that forms between adjacent epithelial cells or endothelial cells. • Tight junctions regulate transport of particles between epithelial cells.
15.16 Tight junctions form selectively permeable barriers between cells • Tight junctions also preserve epithelial cell polarity by serving as a “fence.” • It prevents diffusion of plasma membrane proteins between the apical and basal regions.
15.17 Septate junctions in invertebrates are similar to tight junctions • The septate junction: • is found only in invertebrates • is similar to the vertebrate tight junction • Septate junctions appear as a series of either straight or folded walls (septa) between the plasma membranes of adjacent epithelial cells.
