Cartilage Explained

Cartilage

Cartilage is a resilient and smooth type of connective tissue. It is a semi-transparent and non-porous type of tissue. It is usually covered by a tough and fibrous membrane called perichondrium. In tetrapods, it covers and protects the ends of long bones at the joints as articular cartilage,[1] and is a structural component of many body parts including the rib cage, the neck and the bronchial tubes, and the intervertebral discs. In other taxa, such as chondrichthyans and cyclostomes, it constitutes a much greater proportion of the skeleton.[2] It is not as hard and rigid as bone, but it is much stiffer and much less flexible than muscle. The matrix of cartilage is made up of glycosaminoglycans, proteoglycans, collagen fibers and, sometimes, elastin. It usually grows quicker than bone.

Because of its rigidity, cartilage often serves the purpose of holding tubes open in the body. Examples include the rings of the trachea, such as the cricoid cartilage and carina.

Cartilage is composed of specialized cells called chondrocytes that produce a large amount of collagenous extracellular matrix, abundant ground substance that is rich in proteoglycan and elastin fibers. Cartilage is classified in three types, elastic cartilage, hyaline cartilage and fibrocartilage, which differ in relative amounts of collagen and proteoglycan.

Cartilage does not contain blood vessels or nerves, hence it is insensitive. Some fibrocartilage such as the meniscus of the knee does however have blood supply in part. Nutrition is supplied to the chondrocytes by diffusion. The compression of the articular cartilage or flexion of the elastic cartilage generates fluid flow, which assists the diffusion of nutrients to the chondrocytes. Compared to other connective tissues, cartilage has a very slow turnover of its extracellular matrix and is documented to repair at only a very slow rate relative to other tissues.

Structure

Development

See main article: Chondrogenesis. In embryogenesis, the skeletal system is derived from the mesoderm germ layer. Chondrification (also known as chondrogenesis) is the process by which cartilage is formed from condensed mesenchyme tissue, which differentiates into chondroblasts and begins secreting the molecules (aggrecan and collagen type II) that form the extracellular matrix. In all vertebrates, cartilage is the main skeletal tissue in early ontogenetic stages;[3] [4] in osteichthyans, many cartilaginous elements subsequently ossify through endochondral and perichondral ossification.[5]

Following the initial chondrification that occurs during embryogenesis, cartilage growth consists mostly of the maturing of immature cartilage to a more mature state. The division of cells within cartilage occurs very slowly, and thus growth in cartilage is usually not based on an increase in size or mass of the cartilage itself.[6] It has been identified that non-coding RNAs (e.g. miRNAs and long non-coding RNAs) as the most important epigenetic modulators can affect the chondrogenesis. This also justifies the non-coding RNAs' contribution in various cartilage-dependent pathological conditions such as arthritis, and so on.[7]

Articular cartilage

The articular cartilage function is dependent on the molecular composition of the extracellular matrix (ECM). The ECM consists mainly of proteoglycan and collagens. The main proteoglycan in cartilage is aggrecan, which, as its name suggests, forms large aggregates with hyaluronan and with itself.[8] These aggregates are negatively charged and hold water in the tissue. The collagen, mostly collagen type II, constrains the proteoglycans. The ECM responds to tensile and compressive forces that are experienced by the cartilage.[9] Cartilage growth thus refers to the matrix deposition, but can also refer to both the growth and remodeling of the extracellular matrix. Due to the great stress on the patellofemoral joint during resisted knee extension, the articular cartilage of the patella is among the thickest in the human body.

Function

Mechanical properties

The mechanical properties of articular cartilage in load-bearing joints such as the knee and hip have been studied extensively at macro, micro, and nano-scales. These mechanical properties include the response of cartilage in frictional, compressive, shear and tensile loading. Cartilage is resilient and displays viscoelastic properties.[10]

Since cartilage has interstitial fluid that is free-moving, it makes the material difficult to test. One of the tests commonly used to overcome this obstacle is a confined compression test, which can be used in either a “creep” or “relaxation” mode.[11] [12] In creep mode, the tissue displacement is measured as a function of time under a constant load, and in relaxation mode, the force is measured as a function of time under constant displacement. In creep mode, the tissue displacement is measured as a function of time under a constant load. During this mode, the deformation of the tissue has two main regions. In the first region, the displacement is rapid due to the initial flow of fluid out of the cartilage, and in the second region, the displacement slows down to an eventual constant equilibrium value. Under the commonly used loading conditions, the equilibrium displacement can take hours to reach.

In both the creep mode and the relaxation mode of a confined compression test, a disc of cartilage is placed in an impervious, fluid-filled container and covered with a porous plate that restricts the flow of interstitial fluid to the vertical direction. This test can be used to measure the aggregate modulus of cartilage, which is typically in the range of 0.5 to 0.9 MPa for articular cartilage,[13] and the Young’s Modulus, which is typically 0.45 to 0.80 MPa. The aggregate modulus is “a measure of the stiffness of the tissue at equilibrium when all fluid flow has ceased”, and Young’s modulus is a measure of how much a material strains (changes length) under a given stress.

The confined compression test can also be used to measure permeability, which is defined as the resistance to fluid flow through a material. Higher permeability allows for fluid to flow out of a material’s matrix more rapidly, while lower permeability leads to an initial rapid fluid flow and a slow decrease to equilibrium. Typically, the permeability of articular cartilage is in the range of 10^-15 to 10^-16 m^4/Ns. However, permeability is sensitive to loading conditions and testing location. For example, permeability varies throughout articular cartilage and tends to be highest near the joint surface and lowest near the bone (or “deep zone”). Permeability also decreases under increased loading of the tissue.

Indentation testing is an additional type of test commonly used to characterize cartilage.[14] Indentation testing involves using an indentor (usually <0.8 mm) to measure the displacement of the tissue under constant load. Similar to confined compression testing, it may take hours to reach equilibrium displacement. This method of testing can be used to measure the aggregate modulus, Poisson’s ratio, and permeability of the tissue. Initially, there was a misconception that due to its predominantly water-based composition, cartilage had a Poisson’s ratio of 0.5 and should be modeled as an incompressible material. However, subsequent research has disproven this belief. The Poisson’s ratio of articular cartilage has been measured to be around 0.4 or lower in humans and ranges from 0.46 - 0.5 in bovine subjects.[15]

The mechanical properties of articular cartilage are largely anisotropic, test-dependent, and can be age-dependent. These properties also depend on collagen-proteoglycan interactions and therefore can increase/decrease depending on the total content of water, collagen, glycoproteins, etc. For example, increased glucosaminoglycan content leads to an increase in compressive stiffness, and increased water content leads to a lower aggregate modulus.

Tendon-bone interface

In addition to its role in load-bearing joints, cartilage serves a crucial function as a gradient material between softer tissues and bone. Mechanical gradients are crucial for your body’s function, and for complex artificial structures including joint implants. Interfaces with mismatched material properties lead to areas of high stress concentration which, over the millions of loading cycles experienced by human joins over a lifetime, would eventually lead to failure. For example, the elastic modulus of human bone is roughly 20 GPa while the softer regions of cartilage can be about 0.5 to 0.9 MPa. [16] [17] When there is a smooth gradient of materials properties, however, stresses are distributed evenly across the interface, which puts less wear on each individual part.

The body solves this problem with stiffer, higher modulus layers near bone, with high concentrations of mineral deposits such as hydroxyapatite. Collagen fibers (which provide mechanical stiffness in cartilage) in this region are anchored directly to bones, reducing the possible deformation. Moving closer to soft tissue into the region known as the tidemark, the density of Chondrocytes increases and collagen fibers are rearranged to optimize for stress dissipation and low friction. The outermost layer near the articular surface is known as the superficial zone, which primarily serves as a lubrication region. Here cartilage is characterized by a dense extracellular matrix and is rich in proteoglycans (which dispel and reabsorb water to soften impacts) and thin collagen oriented parallel to the joint surface which have excellent shear resistant properties. [18]

Osteoarthritis and natural aging both have negative effects on cartilage as a whole as well as the proper function of the materials gradient within. The earliest changes are often in the superficial zone, the softest and most lubricating part of the tissue. Degradation of this layer can put additional stresses on deeper layers which are not designed to support the same deformations. Another common effect of aging is increased crosslinking of collagen fibers. This leads to stiffer cartilage as a whole, which again can lead to early failure as stiffer tissue is more susceptible to fatigue based failure. Aging in calcified regions also generally leads to a larger number of mineral deposits, which has a similarly undesired stiffening effect. [19] Osteoarthritis has more extreme effects and can entirely wear down cartilage, causing direct bone-to-bone contact.[20]

Frictional properties

Lubricin, a glycoprotein abundant in cartilage and synovial fluid, plays a major role in bio-lubrication and wear protection of cartilage.[21]

Repair

Cartilage has limited repair capabilities: Because chondrocytes are bound in lacunae, they cannot migrate to damaged areas. Therefore, cartilage damage is difficult to heal. Also, because hyaline cartilage does not have a blood supply, the deposition of new matrix is slow. Over the last years, surgeons and scientists have elaborated a series of cartilage repair procedures that help to postpone the need for joint replacement. A tear of the meniscus of the knee cartilage can often be surgically trimmed to reduce problems.

Biological engineering techniques are being developed to generate new cartilage, using a cellular "scaffolding" material and cultured cells to grow artificial cartilage.[22] Extensive researches have been conducted on freeze-thawed PVA hydrogels as a base material for such a purpose.[23] These gels have exhibited great promises in terms of biocompatibility, wear resistance, shock absorption, friction coefficient, flexibility, and lubrication, and thus are considered superior to polyethylene-based cartilages. A two-year implantation of the PVA hydrogels as artificial meniscus in rabbits showed that the gels remain intact without degradation, fracture, or loss of properties.

Clinical significance

Disease

See main article: Chondropathy. Several diseases can affect cartilage. Chondrodystrophies are a group of diseases, characterized by the disturbance of growth and subsequent ossification of cartilage. Some common diseases that affect the cartilage are listed below.

Tumors made up of cartilage tissue, either benign or malignant, can occur. They usually appear in bone, rarely in pre-existing cartilage. The benign tumors are called chondroma, the malignant ones chondrosarcoma. Tumors arising from other tissues may also produce a cartilage-like matrix, the best-known being pleomorphic adenoma of the salivary glands.

The matrix of cartilage acts as a barrier, preventing the entry of lymphocytes or diffusion of immunoglobulins. This property allows for the transplantation of cartilage from one individual to another without fear of tissue rejection.

Imaging

Cartilage does not absorb X-rays under normal in vivo conditions, but a dye can be injected into the synovial membrane that will cause the x-rays to be absorbed by the dye. The resulting void on the radiographic film between the bone and meniscus represents the cartilage. For In vitro x-ray scans, the outer soft tissue is most likely removed, so the cartilage and air boundary are enough to contrast the presence of cartilage due to the refraction of the x-ray.[26]

Other animals

Cartilaginous fish

Cartilaginous fish (chondrichthyes) or sharks, rays and chimaeras have a skeleton composed entirely of cartilage.

Invertebrate cartilage

Cartilage tissue can also be found among some arthropods such as horseshoe crabs, some mollusks such as marine snails and cephalopods, and some annelids like sabellid polychaetes.

Arthropods

The most studied cartilage in arthropods is the branchial cartilage of Limulus polyphemus. It is a vesicular cell-rich cartilage due to the large, spherical and vacuolated chondrocytes with no homologies in other arthropods. Other type of cartilage found in Limulus polyphemus is the endosternite cartilage, a fibrous-hyaline cartilage with chondrocytes of typical morphology in a fibrous component, much more fibrous than vertebrate hyaline cartilage, with mucopolysaccharides immunoreactive against chondroitin sulfate antibodies. There are homologous tissues to the endosternite cartilage in other arthropods.[27] The embryos of Limulus polyphemus express ColA and hyaluronan in the gill cartilage and the endosternite, which indicates that these tissues are fibrillar-collagen-based cartilage. The endosternite cartilage forms close to Hh-expressing ventral nerve cords and expresses ColA and SoxE, a Sox9 analog. This is also seen in gill cartilage tissue.[28]

Mollusks

In cephalopods, the models used for the studies of cartilage are Octopus vulgaris and Sepia officinalis. The cephalopod cranial cartilage is the invertebrate cartilage that shows more resemblance to the vertebrate hyaline cartilage. The growth is thought to take place throughout the movement of cells from the periphery to the center. The chondrocytes present different morphologies related to their position in the tissue.The embryos of Sepia officinalis express ColAa, ColAb, and hyaluronan in the cranial cartilages and other regions of chondrogenesis. This implies that the cartilage is fibrillar-collagen-based. The Sepia officinalis embryo expresses hh, whose presence causes ColAa and ColAb expression and is also able to maintain proliferating cells undiferentiated. It has been observed that this species presents the expression SoxD and SoxE, analogs of the vertebrate Sox5/6 and Sox9, in the developing cartilage. The cartilage growth pattern is the same as in vertebrate cartilage.

In gastropods, the interest lies in the odontophore, a cartilaginous structure that supports the radula. The most studied species regarding this particular tissue is Busycotypus canaliculatus. The odontophore is a vesicular cell rich cartilage, consisting of vacuolated cells containing myoglobin, surrounded by a low amount of extra cellular matrix containing collagen. The odontophore contains muscle cells along with the chondrocytes in the case of Lymnaea and other mollusks that graze vegetation.

Sabellid polychaetes

The Sabellid polychaetes, or feather duster worms, have cartilage tissue with cellular and matrix specialization supporting their tentacles. They present two distinct extracellular matrix regions. These regions are an acellular fibrous region with a high collagen content, called cartilage-like matrix, and collagen lacking a highly cellularized core, called osteoid-like matrix. The cartilage-like matrix surrounds the osteoid-like matrix. The amount of the acellular fibrous region is variable. The model organisms used in the study of cartilage in sabellid polychaetes are Potamilla sp and Myxicola infundibulum.

Plants and fungi

Vascular plants, particularly seeds, and the stems of some mushrooms, are sometimes called "cartilaginous", although they contain no cartilage.[29]

Further reading

External links

Notes and References

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  2. Book: de Buffrénil . Vivian . de Ricqlès . Armand J . Zylberberg . Louise . Padian . Kevin . Laurin . Michel . Quilhac . Alexandra . Vertebrate skeletal histology and paleohistology . 2021 . CRC Press . Boca Raton, FL . 978-1351189576 . xii + 825 . Firstiton .
  3. Buffrénil . Vivian de . Quilhac . Alexandra . An Overview of the Embryonic Development of the Bony Skeleton . Vertebrate Skeletal Histology and Paleohistology . 2021 . 29–38 . 10.1201/9781351189590-2 . CRC Press. 9781351189590 . 236422314 .
  4. Quilhac . Alexandra . An Overview of Cartilage Histology . Vertebrate Skeletal Histology and Paleohistology . 2021 . 123–146 . 10.1201/9781351189590-7 . CRC Press. 9781351189590 . 236413810 .
  5. Cervantes-Diaz . Fret . Contreras . Pedro . Marcellini . Sylvain . Evolutionary origin of endochondral ossification: the transdifferentiation hypothesis . Development Genes and Evolution . March 2017 . 227 . 2 . 121–127 . 10.1007/s00427-016-0567-y. 27909803 . 21024809 .
  6. Asanbaeva A, Masuda K, Thonar EJ, Klisch SM, Sah RL . Cartilage growth and remodeling: modulation of balance between proteoglycan and collagen network in vitro with beta-aminopropionitrile . Osteoarthritis and Cartilage . 16 . 1 . 1–11 . January 2008 . 17631390 . 10.1016/j.joca.2007.05.019 . free .
  7. Razmara E, Bitaraf A, Yousefi H, Nguyen TH, Garshasbi M, Cho WC, Babashah S . Non-Coding RNAs in Cartilage Development: An Updated Review . International Journal of Molecular Sciences . 20 . 18 . 4475 . September 2019 . 31514268 . 6769748 . 10.3390/ijms20184475 . free .
  8. Chremos A, Horkay F . Coexistence of Crumpling and Flat Sheet Conformations in Two-Dimensional Polymer Networks: An Understanding of Aggrecan Self-Assembly . Physical Review Letters . 131 . 138101 . September 2023 . 13 . 10.1103/PhysRevLett.131.138101 . 37832020 . 2023PhRvL.131m8101C . 263252529 .
  9. Asanbaeva A, Tam J, Schumacher BL, Klisch SM, Masuda K, Sah RL . Articular cartilage tensile integrity: modulation by matrix depletion is maturation-dependent . Archives of Biochemistry and Biophysics . 474 . 1 . 175–82 . June 2008 . 18394422 . 2440786 . 10.1016/j.abb.2008.03.012 .
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  13. Korhonen . R. K. . Laasanen . M. S. . Töyräs . J. . Rieppo . J. . Hirvonen . J. . Helminen . H. J. . Jurvelin . J. S. . 2002 . Comparison of the Equilibrium Response of Articular Cartilage in Unconfined Compression, Confined Compression and Indentation . Journal of Biomechanics . 35 . 7 . 903–909. 10.1016/S0021-9290(02)00052-0 . 12052392 .
  14. Kabir . W. . Di Bella . C. . Choong . P. F. M. . O’Connell . C. D. . 2021 . Assessment of Native Human Articular Cartilage: A Biomechanical Protocol . Cartilage . 13 . 2 Suppl . 427S–437S. 10.1177/1947603520973240 . 33218275 . 8804788 .
  15. Jin . H. . Lewis . J. L. . 2004 . Determination of Poisson's Ratio of Articular Cartilage by Indentation Using Different-Sized Indenters . Journal of Biomechanical Engineering . 126 . 2 . 138–145. 10.1115/1.1688772 .
  16. Handorf . Andrew . Tissue Stiffness Dictates Development, Homeostasis, and Disease Progression . Organogensis . 27 April 2015 . 11 . 1 . 1–15 . 10.1080/15476278.2015.1019687 . 25915734 . 4594591 .
  17. Book: Mansour . Joseph . Biomechanics of Cartilage . MDPI . 66–79 .
  18. Chen . Li . Preparation and Characterization of Biomimetic Functional Scaffold with Gradient Structure for Osteochondral Defect Repair . Bioengineering . 6 February 2023 . 10 . 2 . 213 . 10.3390/bioengineering10020213 . free . 36829707 . 9952804 .
  19. Lotz . Martin . Effects of aging on articular cartilage homeostasis . Bone . 28 March 2012 . 51 . 2 . 241–248 . 10.1016/j.bone.2012.03.023 . 22487298 . 3372644 .
  20. Web site: Osteoarthritis . Mayo Clinic . 13 May 2024.
  21. Rhee DK, Marcelino J, Baker M, Gong Y, Smits P, Lefebvre V, Jay GD, Stewart M, Wang H, Warman ML, Carpten JD . 6 . The secreted glycoprotein lubricin protects cartilage surfaces and inhibits synovial cell overgrowth . The Journal of Clinical Investigation . 115 . 3 . 622–31 . March 2005 . 15719068 . 548698 . 10.1172/JCI22263 .
  22. http://www.cartilage.org International Cartilage Repair Society ICRS
  23. Adelnia. Hossein. Ensandoost. Reza. Shebbrin Moonshi. Shehzahdi. Gavgani. Jaber Nasrollah. Vasafi. Emad Izadi. Ta. Hang Thu. 2022-02-05. Freeze/thawed polyvinyl alcohol hydrogels: Present, past and future. European Polymer Journal. en. 164. 110974. 10.1016/j.eurpolymj.2021.110974. 245576810. 0014-3057. 10072/417476. free.
  24. News: Supplements for osteoarthritis 'do not work' . BBC News . 16 September 2010.
  25. Ansari . Mohammad Y. . Ahmad . Nashrah . Haqqi . Tariq M. . 2018-09-05 . Butein Activates Autophagy Through AMPK/TSC2/ULK1/mTOR Pathway to Inhibit IL-6 Expression in IL-1β Stimulated Human Chondrocytes . Cellular Physiology and Biochemistry . 49 . 3 . 932–946 . 10.1159/000493225 . 30184535 . 52166938 . 1015-8987. free .
  26. http://osteoarthritis.about.com/od/osteoarthritis101/a/cartilage.htm Osteoarthritis
  27. Cole AG, Hall BK . The nature and significance of invertebrate cartilages revisited: distribution and histology of cartilage and cartilage-like tissues within the Metazoa . Zoology . 107 . 4 . 261–73 . 2004 . 16351944 . 10.1016/j.zool.2004.05.001 .
  28. Tarazona OA, Slota LA, Lopez DH, Zhang G, Cohn MJ . The genetic program for cartilage development has deep homology within Bilateria . Nature . 533 . 7601 . 86–9 . May 2016 . 27111511 . 10.1038/nature17398 . 2016Natur.533...86T . 3932905 .
  29. http://eflora.library.usyd.edu.au/glossary/cartilaginous Eflora – Glossary