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小鼠巢蛋白-2与基底膜成分及细胞的结合及其在胚胎和成年组织中的表达表明两种巢蛋白具有互补功能。

Binding of mouse nidogen-2 to basement membrane components and cells and its expression in embryonic and adult tissues suggest complementary functions of the two nidogens.

作者信息

Salmivirta Katriina, Talts Jan F, Olsson Magnus, Sasaki Takako, Timpl Rupert, Ekblom Peter

机构信息

Department of Cell and Molecular Biology, Uppsala University, Uppsala, Sweden.

出版信息

Exp Cell Res. 2002 Oct 1;279(2):188-201. doi: 10.1006/excr.2002.5611.

DOI:10.1006/excr.2002.5611
PMID:12243745
Abstract

Nidogen-1 binds several basement membrane components by well-defined, domain-specific interactions. Organ culture and gene targeting approaches suggest that a high-affinity nidogen-binding site of the laminin gamma1 chain (gamma1III4) is important for kidney development and for nerve guidance. Other proteins may also bind gamma1III4, although human nidogen-2 binds poorly to the mouse laminin gamma1 chain. We therefore characterized recombinant mouse nidogen-2 and its binding to basement membrane proteins and cells. Mouse nidogen-1 and -2 interacted at comparable levels with collagen IV, perlecan, and fibulin-2 and, most notably, also with laminin-1 fragments P1 and gamma1III3-5, which both contain the gamma1III4 module. In embryos, nidogen-2 mRNA was produced by mesenchyme at sites of epithelial-mesenchymal interactions, but the protein was deposited on epithelial basement membranes, as previously shown for nidogen-1. Hence, binding of both nidogens to the epithelial laminin gamma1 chain is dependent on epithelial-mesenchymal interactions. Epidermal growth factor stimulated expression of both nidogens in embryonic submandibular glands. Both nidogens were found in all studied embryonic and adult basement membranes. Nidogen-2 was more adhesive than nidogen-1 for some cell lines and was mainly mediated by alpha3beta1 and alpha6beta1 integrins as shown by antibody inhibition. These findings revealed extensive coregulation of nidogen-1 and -2 expression and much more complementary functions of the two nidogens than previously recognized.

摘要

巢蛋白-1通过明确的、结构域特异性相互作用结合多种基底膜成分。器官培养和基因靶向方法表明,层粘连蛋白γ1链(γ1III4)的高亲和力巢蛋白结合位点对肾脏发育和神经导向很重要。其他蛋白质也可能结合γ1III4,尽管人巢蛋白-2与小鼠层粘连蛋白γ1链的结合能力较差。因此,我们对重组小鼠巢蛋白-2及其与基底膜蛋白和细胞的结合进行了表征。小鼠巢蛋白-1和-2与IV型胶原、基底膜聚糖和纤连蛋白-2的相互作用水平相当,最值得注意的是,它们还与层粘连蛋白-1片段P1和γ1III3-5相互作用,这两个片段都包含γ1III4模块。在胚胎中,巢蛋白-2 mRNA由上皮-间充质相互作用部位的间充质产生,但该蛋白沉积在上皮基底膜上,如先前对巢蛋白-1的研究所示。因此,两种巢蛋白与上皮层粘连蛋白γ1链的结合都依赖于上皮-间充质相互作用。表皮生长因子刺激胚胎下颌下腺中两种巢蛋白的表达。在所有研究的胚胎和成人基底膜中都发现了两种巢蛋白。对于某些细胞系,巢蛋白-2比巢蛋白-1更具黏附性,抗体抑制实验表明,这主要由α3β1和α6β1整合素介导。这些发现揭示了巢蛋白-1和-2表达的广泛共调节,以及这两种巢蛋白比以前认识到更多的互补功能。

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Binding of mouse nidogen-2 to basement membrane components and cells and its expression in embryonic and adult tissues suggest complementary functions of the two nidogens.小鼠巢蛋白-2与基底膜成分及细胞的结合及其在胚胎和成年组织中的表达表明两种巢蛋白具有互补功能。
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