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Plectin
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Plectin is a giant found in nearly all cells which acts as a link between the three main components of the : microfilaments, and intermediate filaments. In addition, plectin links the cytoskeleton to junctions found in the that structurally connect different cells. By holding these different networks together, plectin plays an important role in maintaining the mechanical integrity and properties of tissues.

Structure
Plectin can exist in cells as several alternatively-spliced isoforms, all around 500 kDa and >4000 amino acids. The structure of plectin is thought to be a consisting of a central of connecting two large globular domains (one at each terminus). These globular domains are responsible for connecting plectin to its various cytoskeletal targets. The carboxy-terminal domain is made of 6 highly homologous repeating regions. The subdomain between regions five and six of this domain is known to connect to the intermediate filaments and . At the opposite end of the protein, in the N-terminal domain, a region has been defined as responsible for binding to . In 2004, the exact crystal structure of this -binding domain (ABD) was determined in mice and shown to be composed of two calponin homology (CH) domains. Plectin is expressed in nearly all mammalian tissues. In and , plectin is localized to specialized entities known as Z-discs. Plectin binds several proteins, including , , , fodrin, microtubule-associating proteins, nuclear laminin B, SPTAN1, and ITGB4.

Function
Studies employing a plectin have shed light on the functions of plectin. Pups died 2–3 days after birth, and these mice exhibited marked skin abnormalities, including degeneration of . Skeletal and cardiac muscle tissues were also significantly affected. Cardiac intercalated discs were disintegrated and sarcomeres were irregularly shapen, and intracellular accumulation of aberrant isolated myofibrillar bundles and Z-disc components was also observed. Expression of in muscle cells was strikingly down-regulated. Through the use of gold-immunoelectron microscopy, and immunofluorescence experiments plectin has been found to associate with all three major components of the cytoskeleton. In muscle, plectin binds to the periphery of Z-discs, and along with the intermediate filament protein , may form lateral linkages among neighboring Z-discs. This interaction between plectin and desmin intermediate filaments also appears to facilitate the close association of myofibrils and mitochondria, both at Z-discs and along the remainder the . Plectin also functions to link cytoskeleton to intercellular junctions, such as and , which link intermediate filament networks between cells. Plectin has been revealed to localize to the desmosomes and in vitro studies have shown that it can form bridges between the desmosome protein, and intermediate filaments. In hemidesmosomes plectin has been shown to interact with the β4 subunits of the hemidesmosome plaque and function in a clamp-like manner to link the intermediate filament to the junction.

Clinical significance
Mutations in PLEC have been associated with epidermolysis bullosa simplex with muscular dystrophy. A missense variant of PLEC has been recently proposed as a cause of atrial fibrillation in some populations. Isolated left ventricular non-compaction accompanying epidermolysis bullosa simplex with muscular dystrophy was also noted. Plectin has been proposed as a for pancreatic cancer. Although normally a protein, plectin is expressed on the cell membrane in pancreatic ductal adenocarcinoma (PDAC) and can therefore be used to target PDAC cells.

See also
  • List of target antigens in pemphigus

Further reading
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