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层粘连蛋白片段E8介导的细胞黏附、铺展及神经突刺激作用依赖于其杆状和球状结构域二级和三级结构的维持。

Cell adhesion, spreading and neurite stimulation by laminin fragment E8 depends on maintenance of secondary and tertiary structure in its rod and globular domain.

作者信息

Deutzmann R, Aumailley M, Wiedemann H, Pysny W, Timpl R, Edgar D

机构信息

Institut für Biochemie, Mikrobiologie and Genetik, Universität Regensburg, Federal Republic of Germany.

出版信息

Eur J Biochem. 1990 Jul 31;191(2):513-22. doi: 10.1111/j.1432-1033.1990.tb19151.x.

Abstract

The cell adhesion, spreading and neurite-promoting properties of mouse tumor laminin fragment E8, which contains major site(s) responsible for laminin-cell interactions, were probed by proteolytic degradation, denaturation, synthetic peptides and antibody inhibition. Removal of more than half of the N-terminal portion contributing to the rod-like domain did not effect cell attachment or spreading although neurite-promoting activity was reduced. More extensive degradation of the rod or of the globular domains of E8, or separation of the globule from the rod, also resulted in loss of cell spreading activity although weak attachment was found to an A chain subfragment comprising the globular domain and a short piece of the rod. Exposure of E8 to increasing concentrations of dissociating agents produce an apparently reversible denaturation but an irreversible loss of both attachment and neurite-promoting activities, as did reduction and alkylation of disulfide bonds in the globular domain. Although cell adhesion and spreading were blocked by antibodies to an alpha 6 integrin subunit, neurite outgrowth was unaffected, indicating two distinct receptors for these two activities. Furthermore, a synthetic peptide, the sequence of which is found in the vicinity of adhesion and neurite-promoting sites and previously implicated in neurite growth and cell attachment activities, was found to be inactive. These results indicate that the major cell attachment and neurite-promoting sites of laminin are distinct although both require the native conformation of parts of the rod and the terminal globular domain of the long arm of laminin.

摘要

小鼠肿瘤层粘连蛋白片段E8含有层粘连蛋白与细胞相互作用的主要位点,通过蛋白水解降解、变性、合成肽和抗体抑制等方法对其细胞黏附、铺展和促神经突生长特性进行了探究。去除构成杆状结构域的N端部分的一半以上,虽会降低促神经突生长活性,但不影响细胞附着或铺展。对E8的杆状结构域或球状结构域进行更广泛的降解,或将球状结构与杆状结构分离,也会导致细胞铺展活性丧失,不过发现细胞对包含球状结构域和一小段杆状结构的A链亚片段有较弱的附着。将E8暴露于浓度不断增加的解离剂中会产生明显可逆的变性,但会导致附着和促神经突生长活性的不可逆丧失,对球状结构域中的二硫键进行还原和烷基化处理也会如此。虽然抗α6整合素亚基抗体可阻断细胞黏附和铺展,但对神经突生长没有影响,这表明这两种活性存在两种不同的受体。此外,发现一种合成肽无活性,该肽的序列存在于黏附位点和促神经突生长位点附近,且先前与神经突生长和细胞附着活性有关。这些结果表明,层粘连蛋白的主要细胞附着位点和促神经突生长位点是不同的,尽管两者都需要层粘连蛋白长臂的杆状部分和末端球状结构域的天然构象。

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