The extracellular matrix and cell adhesion
-
Upload
phungxuyen -
Category
Documents
-
view
218 -
download
0
Transcript of The extracellular matrix and cell adhesion
![Page 1: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/1.jpg)
Chapter 15
The extracellular matrix and cell adhesion
ByGeorge Plopper
![Page 2: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/2.jpg)
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
![Page 3: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/3.jpg)
• 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
15.1 Introduction
![Page 4: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/4.jpg)
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.
![Page 5: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/5.jpg)
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.
![Page 6: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/6.jpg)
• 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
![Page 7: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/7.jpg)
• Mutations of collagen genes can lead to a wide range of diseases, from mild wrinkling to brittle bones to fatal blistering of the skin.
15.3 Collagen provides structural support to tissues
![Page 8: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/8.jpg)
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.
![Page 9: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/9.jpg)
• 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
![Page 10: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/10.jpg)
• 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
![Page 11: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/11.jpg)
• 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.
15.4 Fibronectins connect cells to collagenous matrices
![Page 12: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/12.jpg)
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.
![Page 13: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/13.jpg)
• 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
![Page 14: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/14.jpg)
• 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.
15.5 Elastic fibers impart flexibility to tissues
![Page 15: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/15.jpg)
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
![Page 16: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/16.jpg)
• 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
![Page 17: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/17.jpg)
• A large number of proteins bind to laminins, including more than 20 different cell surface receptors.
15.6 Laminins provide an adhesive substrate for cells
![Page 18: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/18.jpg)
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
![Page 19: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/19.jpg)
• 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.
15.7 Vitronectin facilitates targeted cell adhesion during blood clotting
![Page 20: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/20.jpg)
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.
![Page 21: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/21.jpg)
• 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
![Page 22: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/22.jpg)
• 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
15.8 Proteoglycans provide hydration to tissues
![Page 23: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/23.jpg)
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.
![Page 24: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/24.jpg)
• 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
![Page 25: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/25.jpg)
• 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
15.9 Hyaluronan is a glycosaminoglycan enriched in connective tissues
![Page 26: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/26.jpg)
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
![Page 27: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/27.jpg)
• 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
![Page 28: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/28.jpg)
• 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
15.10 Heparan sulfate proteoglycans are cell surface coreceptors
![Page 29: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/29.jpg)
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
![Page 30: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/30.jpg)
• 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
![Page 31: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/31.jpg)
• 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
15.11 The basal lamina is a specialized extracellular matrix
![Page 32: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/32.jpg)
15.12 Proteases degrade extracellular matrix components• Cells must routinely degrade and
replace their extracellular matrix as a normal part of – development – wound healing
![Page 33: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/33.jpg)
• 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
![Page 34: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/34.jpg)
• 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
![Page 35: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/35.jpg)
• 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
![Page 36: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/36.jpg)
• 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.
15.12 Proteases degrade extracellular matrix components
![Page 37: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/37.jpg)
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.
![Page 38: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/38.jpg)
• 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
![Page 39: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/39.jpg)
• 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
![Page 40: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/40.jpg)
• 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.
15.13 Most integrins are receptors for extracellular matrix proteins
![Page 41: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/41.jpg)
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.
![Page 42: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/42.jpg)
• 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
![Page 43: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/43.jpg)
• 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
![Page 44: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/44.jpg)
• 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
![Page 45: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/45.jpg)
• 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.
15.14 Integrin receptors participate in cell signaling
![Page 46: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/46.jpg)
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.
![Page 47: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/47.jpg)
• 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
15.15 Integrins and extracellular matrix molecules play key roles in development
![Page 48: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/48.jpg)
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.
![Page 49: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/49.jpg)
• 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.
15.16 Tight junctions form selectively permeable barriers between cells
![Page 50: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/50.jpg)
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.
![Page 51: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/51.jpg)
• Septate junctions function principally as barriers to paracellular diffusion.
• Septate junctions perform two functions not associated with tight junctions: – they control cell growth and cell shape
during development. • A special set of proteins unique to septate
junctions performs these functions.
15.17 Septate junctions in invertebrates are similar to tight junctions
![Page 52: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/52.jpg)
15.18 Adherens junctions link adjacent cells
• Adherens junctions are a family of related cell surface domains.– They link neighboring cells together.
• Adherens junctions contain transmembrane cadherin receptors.
![Page 53: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/53.jpg)
• The best-known adherens junction is the zonula adherens.– It is located within the junctional
complex that forms between neighboring epithelial cells in some tissues.
• Within the zonula adherens, adaptor proteins called catenins link cadherins to actin filaments.
15.18 Adherens junctions link adjacent cells
![Page 54: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/54.jpg)
15.19 Desmosomes are intermediate filamentbased cell
adhesion complexes• The principal function of
desmosomes is to:– provide structural integrity to sheets
of epithelial cells by linking the intermediate filament networks of cells.
![Page 55: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/55.jpg)
• Desmosomes are components of the junctional complex.
• At least seven proteins have been identified in desmosomes.
• The molecular composition of desmosomes varies in different cell and tissue types.
15.19 Desmosomes are intermediate filament-based cell adhesion complexes
![Page 56: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/56.jpg)
• Desmosomes function as both:– adhesive structures – signal transducing complexes
• Mutations in desmosomal components result in fragile epithelial structures. – These mutations can be lethal,
especially if they affect the organization of the skin.
15.19 Desmosomes are intermediate filament-based cell adhesion complexes
![Page 57: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/57.jpg)
15.20 Hemidesmosomes attach epithelial cells to the basal lamina
• Hemidesmosomes, like desmosomes, provide structural stability to epithelial sheets.
• Hemidesmosomes are found on the basal surface of epithelial cells.– There, they link the extracellular
matrix to the intermediate filament network via transmembrane receptors.
![Page 58: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/58.jpg)
• Hemidesmosomes are structurally distinct from desmosomes.
• They contain at least six unique proteins.
15.20 Hemidesmosomes attach epithelial cells to the basal lamina
![Page 59: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/59.jpg)
• Mutations in hemidesmosome genes give rise to diseases similar to those associated with desmosomal gene mutations.
• The signaling pathways responsible for regulating hemidesmosome assembly are not well understood.
15.20 Hemidesmosomes attach epithelial cells to the basal lamina
![Page 60: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/60.jpg)
15.21 Gap junctions allow direct transfer of molecules between
adjacent cells• Gap junctions are protein
structures that facilitate direct transfer of small molecules between adjacent cells.
• They are found in most animal cells.
![Page 61: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/61.jpg)
• Gap junctions consist of clusters of cylindrical gap junction channels, which:– project outward from the plasma membrane – span a 2-3 nm gap between adjacent cells
• The gap junction channels consist of two halves, called connexons or hemichannels.– Each consists of six protein subunits called
connexins.
15.21 Gap junctions allow direct transfer of molecules between adjacent cells
![Page 62: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/62.jpg)
• Over 20 different connexin genes are found in humans.– These combine to form a variety of
connexon types.
• Gap junctions:– allow for free diffusion of molecules
1200 daltons in size – exclude passage of molecules 2000
daltons
15.21 Gap junctions allow direct transfer of molecules between adjacent cells
![Page 63: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/63.jpg)
• Gap junction permeability is regulated by opening and closing of the gap junction channels, a process called “gating.”
• Gating is controlled by changes in – intracellular pH– calcium ion flux– direct phosphorylation of connexin
subunits
15.21 Gap junctions allow direct transfer of molecules between adjacent cells
![Page 64: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/64.jpg)
• Two additional families of nonconnexin gap junction proteins have been discovered.– This suggests that gap junctions
evolved more than once in the animal kingdom.
15.21 Gap junctions allow direct transfer of molecules between adjacent cells
![Page 65: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/65.jpg)
15.22 Calcium-dependent cadherins mediate adhesion between cells• Cadherins constitute a family of cell
surface transmembrane receptor proteins that are organized into eight groups.
• The best-known group of cadherins is called the “classical cadherins.”– It plays a role in establishing and
maintaining cell-cell adhesion complexes such as the adherens junctions.
![Page 66: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/66.jpg)
• Classical cadherins function as clusters of dimers.
• The strength of adhesion is regulated by varying both:– the number of dimers expressed on
the cell surface – the degree of clustering
15.22 Calcium-dependent cadherins mediate adhesion between cells
![Page 67: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/67.jpg)
• Classical cadherins bind to cytoplasmic adaptor proteins, called catenins.– Catenins link cadherins to the actin
cytoskeleton.
• Cadherin clusters regulate intracellular signaling by forming a cytoskeletal scaffold.– This organizes signaling proteins and their
substrates into a three-dimensional complex.
15.22 Calcium-dependent cadherins mediate adhesion between cells
![Page 68: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/68.jpg)
• Classical cadherins are essential for tissue morphogenesis, primarily by controlling:– specificity of cell-cell adhesion – changes in cell shape and movement
15.22 Calcium-dependent cadherins mediate adhesion between cells
![Page 69: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/69.jpg)
15.23 Calcium-independent NCAMs mediate adhesion between neural
cells• Neural cell adhesion molecules
(NCAMs) are expressed only in neural cells.
• They function primarily as homotypic cell-cell adhesion and signaling receptors.
![Page 70: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/70.jpg)
• Nerve cells express three different types of NCAM proteins.– They arise from alternative splicing of
a single NCAM gene.
15.23 Calcium-independent NCAMs mediate adhesion between neural cells
![Page 71: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/71.jpg)
• Some NCAMs are covalently modified with long chains of polysialic acid (PSA).– This reduces the strength of homotypic
binding.
• This reduced adhesion may be important in developing neurons as they form and break contacts with other neurons.
15.23 Calcium-independent NCAMs mediate adhesion between neural cells
![Page 72: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/72.jpg)
15.24 Selectins control adhesion of circulating immune cells
• Selectins are cell-cell adhesion receptors expressed exclusively on cells in the vascular system.
• Three forms of selectin have been identified:– L-selectin– P-selectin– E-selectin
![Page 73: The extracellular matrix and cell adhesion](https://reader031.fdocuments.in/reader031/viewer/2022021508/586b5b431a28abf3218b4fb0/html5/thumbnails/73.jpg)
• Selectins function to arrest circulating leukocytes in blood vessels so that they can crawl out into the surrounding tissue.
• In a process called discontinuous cell-cell adhesion, selectins on leukocytes bind weakly and transiently to glycoproteins on the endothelial cells.– The leukocytes come to a “rolling stop”
along the blood vessel wall.
15.24 Selectins control adhesion of circulating immune cells