Tight junction

Tight junction
Tight junction
	Diagram of tight junction
Details
Identifiers
Latin	junctio occludens
MeSH	D019108
TH	H1.00.01.1.02007
FMA	67397
	Anatomical terminology [ edit on Wikidata]

Last updated May 08, 2024

Tight junctions, also known as occluding junctions or zonulae occludentes (singular, zonula occludens), are multiprotein junctional complexes whose canonical function is to prevent leakage of solutes and water and seals between the epithelial cells.^[1] They also play a critical role maintaining the structure and permeability of endothelial cells.^[1] Tight junctions may also serve as leaky pathways by forming selective channels for small cations, anions, or water. The corresponding junctions that occur in invertebrates are septate junctions.

Structure

Tight junctions are composed of a branching network of sealing strands, each strand acting independently from the others. Therefore, the efficiency of the junction in preventing ion passage increases exponentially with the number of strands. Each strand is formed from a row of transmembrane proteins embedded in both plasma membranes, with extracellular domains joining one another directly. There are at least 40 different proteins composing the tight junctions.^[2] These proteins consist of both transmembrane and cytoplasmic proteins. The three major transmembrane proteins are occludin, claudins, and junction adhesion molecule (JAM) proteins. These associate with different peripheral membrane proteins such as ZO-1 located on the intracellular side of plasma membrane, which anchor the strands to the actin component of the cytoskeleton.^[3] In this way, tight junctions join together the cytoskeletons of adjacent cells. Investigation using freeze-fracture methods in electron microscopy is ideal for revealing the lateral extent of tight junctions in cell membranes and has been useful in showing how tight junctions are formed.^[4]

Occludin was the first integral membrane protein to be identified. It has a molecular weight of ~60kDa. It consists of four transmembrane domains and both the N-terminus and the C-terminus of the protein are intracellular. It forms two extracellular loops and one intracellular loop. These loops help regulate paracellular permeability.^[5] Occludin also plays a key role in cellular structure and barrier function.^[6]
Claudins were discovered after occludin and are a family of over 27 different members in mammals.^[7] They have a molecular weight of ~20kDa. They have a structure similar to that of occludin in that they have four transmembrane domains and similar loop structure. They are understood to be the backbone of tight junctions and play a significant role in the tight junction's ability to seal the paracellular space.^[8]
Junctional Adhesion Molecules (JAM) are part of the immunoglobulin superfamily. They have a molecular weight of ~40 to 48 kDa.^[9] Their structure differs from that of the other integral membrane proteins in that they only have one transmembrane domain instead of four. It helps to regulate the paracellular pathway function of tight junctions and is also involved in helping to maintain cell polarity.^[10]
Angulins were discovered in 2011 by visual screening of proteins which localize at tricellular tight junctions.^[11] There are three members of angulins, Angulin-1/LSR, Angulin-2/ILDR1, and Angulin-3/ILDR2. Similar to JAMs, angulins are single-transmembrane proteins. All angulins have one immunoglobulin-like domain in the extracellular region and one PDZ-binding motif at the carboxy-terminus. They are responsible for establishment of tricellular tight junctions and regulate the paracellular barrier function.^[12]

Functions

Tight junctions provide endothelial and epithelial cells with barrier function, which can be further subdivided into protective barriers and functional barriers serving purposes such as material transport and maintenance of osmotic balance.^[13]

Tight junctions prevent the passage of molecules and ions through the intercellular space of adjacent cells, so materials must actually enter the cells (by diffusion or active transport) in order to pass through the tissue. The constrained intracellular pathway exacted by the tight junction barrier system allows precise control over which substances can pass through a particular tissue (e.g. the blood–brain barrier). At the present time, it is still unclear whether the control is active or passive and how these pathways are formed. In one study for paracellular transport across the tight junction in kidney proximal tubule, a dual pathway model was proposed, consisting of large slit breaks formed by infrequent discontinuities in the tight junction complex and numerous small circular pores.^[14]

Tight junctions also help maintain the apicobasal polarity of cells by preventing the lateral diffusion of integral membrane proteins between the apical and lateral/basal surfaces, allowing the specialized functions of each surface (for example receptor-mediated endocytosis at the apical surface and exocytosis at the basolateral surface) to be preserved. This allows polarized transcellular transport and specialized functions of apical and basolateral membranes.

Classification

Epithelia are classed as "tight" or "leaky", depending on the ability of the tight junctions to prevent water and solute movement:^[15]

Tight epithelia have tight junctions that prevent most movement between cells. Examples of tight epithelia include the distal convoluted tubule, the collecting duct of the nephron in the kidney, and the bile ducts ramifying through liver tissue. Other examples are the blood-brain barrier and the blood cerebrospinal fluid barrier
Leaky epithelia do not have these tight junctions or have less complex tight junctions. For instance, the tight junction in the kidney proximal tubule, a very leaky epithelium, has only two to three junctional strands, and these strands exhibit infrequent large slit breaks.

Related Research Articles

Epithelium or epithelial tissue is a thin, continuous, protective layer of compactly packed cells with little extracellular matrix. Epithelial tissues line the outer surfaces of organs and blood vessels throughout the body, as well as the inner surfaces of cavities in many internal organs. An example is the epidermis, the outermost layer of the skin. Epithelial tissue is one of the four basic types of animal tissue, along with connective tissue, muscle tissue and nervous tissue. These tissues also lack blood or lymph supply. The tissue is supplied by nerves.

Cell adhesion is the process by which cells interact and attach to neighbouring cells through specialised molecules of the cell surface. This process can occur either through direct contact between cell surfaces such as cell junctions or indirect interaction, where cells attach to surrounding extracellular matrix, a gel-like structure containing molecules released by cells into spaces between them. Cells adhesion occurs from the interactions between cell-adhesion molecules (CAMs), transmembrane proteins located on the cell surface. Cell adhesion links cells in different ways and can be involved in signal transduction for cells to detect and respond to changes in the surroundings. Other cellular processes regulated by cell adhesion include cell migration and tissue development in multicellular organisms. Alterations in cell adhesion can disrupt important cellular processes and lead to a variety of diseases, including cancer and arthritis. Cell adhesion is also essential for infectious organisms, such as bacteria or viruses, to cause diseases.

Cell junctions or junctional complexes are a class of cellular structures consisting of multiprotein complexes that provide contact or adhesion between neighboring cells or between a cell and the extracellular matrix in animals. They also maintain the paracellular barrier of epithelia and control paracellular transport. Cell junctions are especially abundant in epithelial tissues. Combined with cell adhesion molecules and extracellular matrix, cell junctions help hold animal cells together.

Claudins are a family of proteins which, along with occludin, are the most important components of the tight junctions. Tight junctions establish the paracellular barrier that controls the flow of molecules in the intercellular space between the cells of an epithelium. They have four transmembrane domains, with the N-terminus and the C-terminus in the cytoplasm.

Transcytosis is a type of transcellular transport in which various macromolecules are transported across the interior of a cell. Macromolecules are captured in vesicles on one side of the cell, drawn across the cell, and ejected on the other side. Examples of macromolecules transported include IgA, transferrin, and insulin. While transcytosis is most commonly observed in epithelial cells, the process is also present elsewhere. Blood capillaries are a well-known site for transcytosis, though it occurs in other cells, including neurons, osteoclasts and M cells of the intestine.

The epithelial sodium channel(ENaC), (also known as amiloride-sensitive sodium channel) is a membrane-bound ion channel that is selectively permeable to sodium ions (Na⁺). It is assembled as a heterotrimer composed of three homologous subunits α or δ, β, and γ, These subunits are encoded by four genes: SCNN1A, SCNN1B, SCNN1G, and SCNN1D. The ENaC is involved primarily in the reabsorption of sodium ions at the collecting ducts of the kidney's nephrons. In addition to being implicated in diseases where fluid balance across epithelial membranes is perturbed, including pulmonary edema, cystic fibrosis, COPD and COVID-19, proteolyzed forms of ENaC function as the human salt taste receptor.

<span class="mw-page-title-main">Occludin</span> Mammalian protein found in Homo sapiens

Occludin is a transmembrane protein that regulates the permeability of epithelial and endothelial barriers. It was first identified in epithelial cells as a 65 kDa integral plasma-membrane protein localized at the tight junctions. Together with Claudins, and zonula occludens-1 (ZO-1), occludin has been considered a staple of tight junctions, and although it was shown to regulate the formation, maintenance, and function of tight junctions, its precise mechanism of action remained elusive and most of its actions were initially attributed to conformational changes following selective phosphorylation, and its redox-sensitive dimerization. However, mounting evidence demonstrated that occludin is not only present in epithelial/endothelial cells, but is also expressed in large quantities in cells that do not have tight junctions but have very active metabolism: pericytes, neurons and astrocytes, oligodendrocytes, dendritic cells, monocytes/macrophages lymphocytes, and myocardium. Recent work, using molecular modeling, supported by biochemical and live-cell experiments in human cells demonstrated that occludin is a NADH oxidase that influences critical aspects of cell metabolism like glucose uptake, ATP production and gene expression. Furthermore, manipulation of occludin content in human cells is capable of influencing the expression of glucose transporters, and the activation of transcription factors like NFkB, and histone deacetylases like sirtuins, which proved capable of diminishing HIV replication rates in infected human macrophages under laboratory conditions.

Paracellular transport refers to the transfer of substances across an epithelium by passing through the intercellular space between the cells. It is in contrast to transcellular transport, where the substances travel through the cell, passing through both the apical membrane and basolateral membrane.

Zonula occludens-1 ZO-1, also known as Tight junction protein-1 is a 220-kD peripheral membrane protein that is encoded by the TJP1 gene in humans. It belongs to the family of zonula occludens proteins, which are tight junction-associated proteins and of which, ZO-1 is the first to be cloned. It was first isolated in 1986 by Stevenson and Goodenough using a monoclonal antibody raised in rodent liver to recognise a 225-kD polypeptide in whole liver homogenates and in tight junction-enriched membrane fractions. It has a role as a scaffold protein which cross-links and anchors Tight Junction (TJ) strand proteins, which are fibril-like structures within the lipid bilayer, to the actin cytoskeleton.

Claudin-1 is a protein that in humans is encoded by the CLDN1 gene. It belongs to the group of claudins.

Claudin-5 is a protein that in humans is encoded by the CLDN5 gene. It belongs to the group of claudins.

Claudin 3, also known as CLDN3, is a protein which in humans is encoded by the CLDN3 gene. It is a member of the claudin protein family.

Claudin-2 is a protein that in humans is encoded by the CLDN2 gene. It belongs to the group of claudins.

Claudin-14 is a protein that in humans is encoded by the CLDN14 gene. It belongs to a related family of proteins called claudins.

Claudin-15 is a protein that in humans is encoded by the CLDN15 gene. It belongs to the group of claudins. Among its related pathways are Blood-Brain Barrier and Immune Cell Transmigration: VCAM-1/CD106 Signaling Pathways and Tight junction. GO annotations related to this gene include identical protein binding and structural molecule activity. An important paralog of this gene is CLDN10.

<span class="mw-page-title-main">Intestinal epithelium</span> Single-cell layer lining the intestines

The intestinal epithelium is the single cell layer that forms the luminal surface (lining) of both the small and large intestine (colon) of the gastrointestinal tract. Composed of simple columnar epithelium its main functions are absorption, and secretion. Useful substances are absorbed into the body, and the entry of harmful substances is restricted. Secretions include mucins, and peptides.

Cell–cell interaction refers to the direct interactions between cell surfaces that play a crucial role in the development and function of multicellular organisms. These interactions allow cells to communicate with each other in response to changes in their microenvironment. This ability to send and receive signals is essential for the survival of the cell. Interactions between cells can be stable such as those made through cell junctions. These junctions are involved in the communication and organization of cells within a particular tissue. Others are transient or temporary such as those between cells of the immune system or the interactions involved in tissue inflammation. These types of intercellular interactions are distinguished from other types such as those between cells and the extracellular matrix. The loss of communication between cells can result in uncontrollable cell growth and cancer.

<span class="mw-page-title-main">Septate junction</span>

Septate junctions are intercellular junctions found in invertebrate epithelial cells, appearing as ladder-like structures under electron microscopy. They are thought to provide structural strength and a barrier to solute diffusion through the intercellular space. They are considered somewhat analogous to the (vertebrate) tight junctions; however, tight and septate junctions are different in many ways. Known insect homologues of tight junction components are components of conserved signalling pathways that localize to either adherens junctions, the subapical complex, or the marginal zone. Recent studies show that septate junctions are also identified in the myelinated nerve fibers of the vertebrates.

The internal surface of the uterus is lined by uterine epithelial cells which undergo dramatic changes during pregnancy. The role of the uterine epithelial cells is to selectively allow the blastocyst to implant at a specific time. All other times of the cycle, these uterine epithelial cells are refractory to blastocyst implantation. Uterine epithelial cells have a similar structure in most species and the changes which occur in the uterine epithelial cells at the time of blastocyst implantation are also conserved among most species.

Tight junction proteins are molecules situated at the tight junctions of epithelial, endothelial and myelinated cells. This multiprotein junctional complex has a regulatory function in passage of ions, water and solutes through the paracellular pathway. It can also coordinate the motion of lipids and proteins between the apical and basolateral surfaces of the plasma membrane. Thereby tight junction conducts signaling molecules, that influence the differentiation, proliferation and polarity of cells. So tight junction plays a key role in maintenance of osmotic balance and trans-cellular transport of tissue specific molecules. Nowadays is known more than 40 different proteins, that are involved in these selective TJ channels.

References

1 2 Bhat, Ajaz A.; Uppada, Srijayaprakash; Achkar, Iman W.; Hashem, Sheema; Yadav, Santosh K.; Shanmugakonar, Muralitharan; Al-Naemi, Hamda A.; Haris, Mohammad; Uddin, Shahab (2019). "Tight Junction Proteins and Signaling Pathways in Cancer and Inflammation: A Functional Crosstalk". Frontiers in Physiology. 9: 1942. doi: 10.3389/fphys.2018.01942 . ISSN 1664-042X. PMC 6351700 . PMID 30728783.
↑ Itallie, Christina M. Van; Anderson, James M. (2009-08-01). "Physiology and Function of the Tight Junction". Cold Spring Harbor Perspectives in Biology. 1 (2): a002584. doi:10.1101/cshperspect.a002584. ISSN 1943-0264. PMC 2742087 . PMID 20066090.
↑ Anderson, JM; Van Itallie, CM (August 2009). "Physiology and function of the tight junction". Cold Spring Harb Perspect Biol. 1 (2): a002584. doi:10.1101/cshperspect.a002584. PMC 2742087 . PMID 20066090.
↑ Chalcroft, J. P.; Bullivant, S (1970). "An interpretation of liver cell membrane and junction structure based on observation of freeze-fracture replicas of both sides of the fracture". The Journal of Cell Biology. 47 (1): 49–60. doi:10.1083/jcb.47.1.49. PMC 2108397 . PMID 4935338.
↑ Wolburg, Hartwig; Lippoldt, Andrea; Ebnet, Klaus (2006), "Tight Junctions and the Blood-Brain Barrier", Tight Junctions, Springer US, pp. 175–195, doi:10.1007/0-387-36673-3_13, ISBN 9780387332017
↑ Liu, Wei-Ye; Wang, Zhi-Bin; Zhang, Li-Chao; Wei, Xin; Li, Ling (2012-06-12). "Tight Junction in Blood-Brain Barrier: An Overview of Structure, Regulation, and Regulator Substances". CNS Neuroscience & Therapeutics. 18 (8): 609–615. doi:10.1111/j.1755-5949.2012.00340.x. ISSN 1755-5930. PMC 6493516 . PMID 22686334.
↑ Schneeberger, Eveline E.; Lynch, Robert D. (June 2004). "The tight junction: a multifunctional complex" (PDF). American Journal of Physiology. Cell Physiology. 286 (6): C1213–C1228. doi:10.1152/ajpcell.00558.2003. ISSN 0363-6143. PMID 15151915. S2CID 1725292. Archived from the original (PDF) on 2019-02-22.
↑ Mitic, Laura L.; Van Itallie, Christina M.; Anderson, James M. (August 2000). "Molecular Physiology and Pathophysiology of Tight Junctions I. Tight junction structure and function: lessons from mutant animals and proteins" (PDF). American Journal of Physiology. Gastrointestinal and Liver Physiology. 279 (2): G250–G254. doi:10.1152/ajpgi.2000.279.2.g250. ISSN 0193-1857. PMID 10915631. S2CID 32634345. Archived from the original (PDF) on 2019-03-09.
↑ Ebnet, Klaus (2017-10-01). "Junctional Adhesion Molecules (JAMs): Cell Adhesion Receptors With Pleiotropic Functions in Cell Physiology and Development". Physiological Reviews. 97 (4): 1529–1554. doi:10.1152/physrev.00004.2017. ISSN 0031-9333. PMID 28931565. S2CID 10846721.
↑ Luissint, Anny-Claude; Artus, Cédric; Glacial, Fabienne; Ganeshamoorthy, Kayathiri; Couraud, Pierre-Olivier (2012-11-09). "Tight junctions at the blood brain barrier: physiological architecture and disease-associated dysregulation". Fluids and Barriers of the CNS. 9 (1): 23. doi: 10.1186/2045-8118-9-23 . ISSN 2045-8118. PMC 3542074 . PMID 23140302.
↑ Masuda, Sayuri; Oda, Yukako; Sasaki, Hiroyuki; Ikenouchi, Junichi; Higashi, Tomohito; Akashi, Masaya; Nishi, Eiichiro; Furuse, Mikio (2011-02-15). "LSR definescell corners for tricellular tight junction formation in epithelial cells". Journal of Cell Science. 124 (Part 4): 548–555. doi: 10.1242/jcs.072058 . PMID 21245199.
↑ Higashi, Tomohito; Miller, Ann (2017-07-15). "Tricellular junctions: how to build junctions at the TRICkiest points of epithelial cells". Molecular Biology of the Cell. 28 (15): 2023–2034. doi:10.1091/mbc.E16-10-0697. ISSN 1939-4586. PMC 5509417 . PMID 28705832.
↑ Department, Biology. "Tight Junctions (and other cellular connections)". Davidson College. Retrieved 2015-01-12.
↑ Guo, P; Weinstein, AM; Weinbaum, S (Aug 2003). "A dual-pathway ultrastructural model for the tight junction of rat proximal tubule epithelium" (PDF). American Journal of Physiology. Renal Physiology. 285 (2): F241–57. doi:10.1152/ajprenal.00331.2002. PMID 12670832. S2CID 22824832. Archived from the original (PDF) on 2019-02-22.
↑ Department, Biology. "Tight Junctions and other cellular connections". Davidson College. Retrieved 2013-09-20.

External links

An Overview of the Tight Junction at Zonapse.Net
Occludin in Focus at Zonapse.Net
Tight+Junctions at the U.S. National Library of Medicine Medical Subject Headings (MeSH)
Histology image: 20502loa – Histology Learning System at Boston University

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[:0-1] 1 2 Bhat, Ajaz A.; Uppada, Srijayaprakash; Achkar, Iman W.; Hashem, Sheema; Yadav, Santosh K.; Shanmugakonar, Muralitharan; Al-Naemi, Hamda A.; Haris, Mohammad; Uddin, Shahab (2019). "Tight Junction Proteins and Signaling Pathways in Cancer and Inflammation: A Functional Crosstalk". Frontiers in Physiology. 9: 1942. doi: 10.3389/fphys.2018.01942 . ISSN 1664-042X. PMC 6351700 . PMID 30728783.

[2] Itallie, Christina M. Van; Anderson, James M. (2009-08-01). "Physiology and Function of the Tight Junction". Cold Spring Harbor Perspectives in Biology. 1 (2): a002584. doi:10.1101/cshperspect.a002584. ISSN 1943-0264. PMC 2742087 . PMID 20066090.

[Anderson2009-3] Anderson, JM; Van Itallie, CM (August 2009). "Physiology and function of the tight junction". Cold Spring Harb Perspect Biol. 1 (2): a002584. doi:10.1101/cshperspect.a002584. PMC 2742087 . PMID 20066090.

[4] Chalcroft, J. P.; Bullivant, S (1970). "An interpretation of liver cell membrane and junction structure based on observation of freeze-fracture replicas of both sides of the fracture". The Journal of Cell Biology. 47 (1): 49–60. doi:10.1083/jcb.47.1.49. PMC 2108397 . PMID 4935338.

[5] Wolburg, Hartwig; Lippoldt, Andrea; Ebnet, Klaus (2006), "Tight Junctions and the Blood-Brain Barrier", Tight Junctions, Springer US, pp. 175–195, doi:10.1007/0-387-36673-3_13, ISBN 9780387332017

[6] Liu, Wei-Ye; Wang, Zhi-Bin; Zhang, Li-Chao; Wei, Xin; Li, Ling (2012-06-12). "Tight Junction in Blood-Brain Barrier: An Overview of Structure, Regulation, and Regulator Substances". CNS Neuroscience & Therapeutics. 18 (8): 609–615. doi:10.1111/j.1755-5949.2012.00340.x. ISSN 1755-5930. PMC 6493516 . PMID 22686334.

[7] Schneeberger, Eveline E.; Lynch, Robert D. (June 2004). "The tight junction: a multifunctional complex" (PDF). American Journal of Physiology. Cell Physiology. 286 (6): C1213–C1228. doi:10.1152/ajpcell.00558.2003. ISSN 0363-6143. PMID 15151915. S2CID 1725292. Archived from the original (PDF) on 2019-02-22.

[8] Mitic, Laura L.; Van Itallie, Christina M.; Anderson, James M. (August 2000). "Molecular Physiology and Pathophysiology of Tight Junctions I. Tight junction structure and function: lessons from mutant animals and proteins" (PDF). American Journal of Physiology. Gastrointestinal and Liver Physiology. 279 (2): G250–G254. doi:10.1152/ajpgi.2000.279.2.g250. ISSN 0193-1857. PMID 10915631. S2CID 32634345. Archived from the original (PDF) on 2019-03-09.

[9] Ebnet, Klaus (2017-10-01). "Junctional Adhesion Molecules (JAMs): Cell Adhesion Receptors With Pleiotropic Functions in Cell Physiology and Development". Physiological Reviews. 97 (4): 1529–1554. doi:10.1152/physrev.00004.2017. ISSN 0031-9333. PMID 28931565. S2CID 10846721.

[10] Luissint, Anny-Claude; Artus, Cédric; Glacial, Fabienne; Ganeshamoorthy, Kayathiri; Couraud, Pierre-Olivier (2012-11-09). "Tight junctions at the blood brain barrier: physiological architecture and disease-associated dysregulation". Fluids and Barriers of the CNS. 9 (1): 23. doi: 10.1186/2045-8118-9-23 . ISSN 2045-8118. PMC 3542074 . PMID 23140302.

[11] Masuda, Sayuri; Oda, Yukako; Sasaki, Hiroyuki; Ikenouchi, Junichi; Higashi, Tomohito; Akashi, Masaya; Nishi, Eiichiro; Furuse, Mikio (2011-02-15). "LSR definescell corners for tricellular tight junction formation in epithelial cells". Journal of Cell Science. 124 (Part 4): 548–555. doi: 10.1242/jcs.072058 . PMID 21245199.

[12] Higashi, Tomohito; Miller, Ann (2017-07-15). "Tricellular junctions: how to build junctions at the TRICkiest points of epithelial cells". Molecular Biology of the Cell. 28 (15): 2023–2034. doi:10.1091/mbc.E16-10-0697. ISSN 1939-4586. PMC 5509417 . PMID 28705832.

[13] Department, Biology. "Tight Junctions (and other cellular connections)". Davidson College. Retrieved 2015-01-12.

[pmid12670832-14] Guo, P; Weinstein, AM; Weinbaum, S (Aug 2003). "A dual-pathway ultrastructural model for the tight junction of rat proximal tubule epithelium" (PDF). American Journal of Physiology. Renal Physiology. 285 (2): F241–57. doi:10.1152/ajprenal.00331.2002. PMID 12670832. S2CID 22824832. Archived from the original (PDF) on 2019-02-22.

[15] Department, Biology. "Tight Junctions and other cellular connections". Davidson College. Retrieved 2013-09-20.

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v t e Proteins of epithelium
Lateral/cell–cell	Cell adhesion molecules: Adherens junction Cadherin Desmosome Desmoglein Ion channels: Gap junction/Connexon Connexin Cytoskeleton: Desmosome Desmoplakin Plakoglobin Tonofibril other membrane proteins: Tight junction Claudin Occludin MARVELD2
Basal/cell–matrix	Basal lamina Hemidesmosome/Tonofibril Focal adhesion Costamere
Apical	Cilia/Kinocilium Microvilli/Stereocilia (STRC)