|
T-cadherin also known as cadherin 13, H-cadherin (heart) (CDH13) is a unique member of cadherin superfamily because it lacks the transmembrane and cytoplasmic domains and is anchored to the cells membrane through the GPI anchor. Classical cadherins are necessary for cell–cell contacts, dynamic regulation of morphogenetic processes in embryos and tissue integrity in adult organism. Cadherins function as membrane receptors mediating outside-in signals, activating small GTPases and beta-catenin/Wnt pathway, and resulting in dynamic cytoskeleton reorganization and changes in the phenotype. T-cadherin is a GPI-anchored member of cadherin superfamily, which lacks a direct contact with cytoskeleton and therefore is not involved in cell–cell adhesion. It is involved in low density lipoproteins (LDL) hormone-like effects on Ca2+-mobilization and increased cell migration as well as phenotype changes. Exact signaling partners and adapter proteins for T-cadherin remain to be elucidated. ==Mediation of intracellular signaling in vascular cells== Though T-cadherin can mediate weak homophilic adhesion in aggregation assays ''in vitro'', the lack of intracellular domain suggests that Т-cadherin is not involved in stable сеll-сеll adhesion. ''In vivo'' T-cadherin was detected оn the apical сеll surface of the chick interstinal epithelium. In cultures of transfected MDCS cells, T-cadherin was also expressed apically, whereas N-cadherin located basolaterally corresponded to the zone of сеll contacts. Тhе apical сеll surface distribution of Т-cadherin was proposed to possibly endow Т-cadherin with recognition functions. In confluent cultures of vascular cells, Т-cadherin was distributed equally over the entire сеll surface, in contrast to VE-cadherin, which was restricted to the сеll junctions. In migrating vascular cells, Т-cadherin was located at the leading edge as revealed by confocal microscopy. The distribution of Т-cadherin оn the cell membrane is restricted to lipid rafts where it co-localizes with signal-transducing molecules. These data strongly implicates Т-cadherin in intracellular signaling rather than adhesion. Studying signaling effects of low density lipoproteins (LDL) in vascular smooth muscles (VSMCs), T-cadherin was isolated and identified as new LDL receptor using human aortic media and the ligand-blotting method. The properties of T-cadherin as an LDL receptor were markedly different from the presently known types of LDL receptors. LDL binding to T-cadherin leads to the activation of Erk 1/2 tyrosine kinase and the nuclear translocation of NF-kappaB. Т-cadherin overexpression in ECs facilitates spontaneous сеll migration, formation of stress fibers and change of the phenotype from quiescent to promigratory. Т-cadherin expression results in LDL-induced migration of T-cadherin expressing cells compared to control. It is likely that Т-cadherin regulates сеll migration and phenotype via activation of small G-proteins with subsequent actin reorganization. RhoA/ROCK activation is necessary for сеll contraction, stress fiber assembly and inhibition of spreading, while Rac is required for the formation of membrane protrusions and actin-rich lamellopodia at the leading edge of migrating cells. 抄文引用元・出典: フリー百科事典『 ウィキペディア(Wikipedia)』 ■ウィキペディアで「T-cadherin」の詳細全文を読む スポンサード リンク
|