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M-钙黏蛋白介导的成肌小鼠细胞中的细胞黏附以及与连环蛋白的复合物形成。

M-cadherin-mediated cell adhesion and complex formation with the catenins in myogenic mouse cells.

作者信息

Kuch C, Winnekendonk D, Butz S, Unvericht U, Kemler R, Starzinski-Powitz A

机构信息

Institut der Anthropologie und Humangenetik für Biologen, Johann Wolfgang Goethe Universität, Frankfurt am Main, Germany.

出版信息

Exp Cell Res. 1997 May 1;232(2):331-8. doi: 10.1006/excr.1997.3519.

DOI:10.1006/excr.1997.3519
PMID:9168809
Abstract

M-cadherin is a member of the multigene family of calcium-dependent intercellular adhesion molecules, the cadherins, which are involved in morphogenetic processes. Amino acid comparisons between M-cadherin and E-, N-, and P-cadherin suggested that M-cadherin diverged phylogenetically very early from these classical cadherins. It has been shown that M-cadherin is expressed in prenatal and adult skeletal muscle. In the cerebellum, M-cadherin is present in an adherens-type junction which differs in its molecular composition from the E-cadherin-mediated adherens-type junctions. These and other findings raised the question of whether M-cadherin and the classical cadherins share basic biochemical properties, notably the calcium-dependent resistance to proteolysis, mediation of calcium-dependent intercellular adhesion, and the capability to form M-cadherin complexes with the catenins. Here we show that M-cadherin is resistant to trypsin digestion in the presence of calcium ions but at lower trypsin concentrations than E-cadherin. When ectopically expressed in LMTK- cells, M-cadherin mediated calcium-dependent cell aggregation. Finally, M-cadherin was capable of forming two distinct cytoplasmic complexes in myogenic cells, either with alpha-catenin/beta-catenin or with alpha-catenin/plakoglobin, as E-and N-cadherin, for example, have previously been shown to form. The relative amount of these complexes changed during differentiation from C2C12 myoblasts to myotubes, although the molecular composition of each complex was unaffected during differentiation. These results demonstrate that M-cadherin shares important features with the classical cadherins despite its phylogenetic divergence.

摘要

M-钙黏蛋白是钙依赖性细胞间黏附分子多基因家族(钙黏蛋白家族)的成员之一,该家族参与形态发生过程。M-钙黏蛋白与E-、N-和P-钙黏蛋白之间的氨基酸比较表明,M-钙黏蛋白在系统发育上很早就与这些经典钙黏蛋白分道扬镳。研究表明,M-钙黏蛋白在产前和成年骨骼肌中均有表达。在小脑中,M-钙黏蛋白存在于一种黏附连接中,其分子组成与E-钙黏蛋白介导的黏附连接不同。这些发现以及其他研究结果引发了一个问题,即M-钙黏蛋白与经典钙黏蛋白是否具有共同的基本生化特性,特别是对蛋白水解的钙依赖性抗性、钙依赖性细胞间黏附的介导作用以及与连环蛋白形成M-钙黏蛋白复合物的能力。在这里,我们表明,在钙离子存在的情况下,M-钙黏蛋白对胰蛋白酶消化具有抗性,但所需的胰蛋白酶浓度低于E-钙黏蛋白。当在LMTK-细胞中异位表达时,M-钙黏蛋白介导钙依赖性细胞聚集。最后,M-钙黏蛋白能够在成肌细胞中形成两种不同的细胞质复合物,一种与α-连环蛋白/β-连环蛋白形成,另一种与α-连环蛋白/桥粒斑蛋白形成,例如,先前已证明E-钙黏蛋白和N-钙黏蛋白也能形成这样的复合物。从C2C12成肌细胞分化为肌管的过程中,这些复合物的相对量发生了变化,尽管每个复合物的分子组成在分化过程中未受影响。这些结果表明,尽管M-钙黏蛋白在系统发育上有所分化,但它与经典钙黏蛋白具有重要的共同特征。

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