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心脏发育过程中微纤维状纤维连接蛋白-1和纤维连接蛋白-2的超微结构定位表明分子关联发生了转变。

Ultrastructural localization of microfibrillar fibulin-1 and fibulin-2 during heart development indicates a switch in molecular associations.

作者信息

Miosge N, Sasaki T, Chu M L, Herken R, Timpl R

机构信息

Abteilung Histologie, Universität Göttingen, Germany.

出版信息

Cell Mol Life Sci. 1998 Jun;54(6):606-13. doi: 10.1007/s000180050188.

Abstract

The microfibrillar proteins fibulin-1 and fibulin-2 were previously identified as prominent components of the endocardial cushion tissue (ECT) during heart development and shown to persist in adult valves and septa. Immunogold staining has now been used to compare their localization in embryonic (days 9-11) and adult mouse heart with that of fibronectin and the chondroitin sulphate proteoglycan versican. All four proteins were deposited in the ECT, which consists of a hyaluronan-rich, mainly unstructured matrix, but were barely detectable in myocardial basement membranes or within endocardial cells. Digestion with hyaluronate lyase selectively released the fibulins and versican but not fibronectin from the ECT. Yet neither of the two fibulins bound to hyaluronan in solid-phase assays, in contrast to versican. In the adult heart valve, all four proteins could be detected close to cross-striated collagen fibrils or microfibrils, but only versican was lost upon exposure to hyaluronate lyase. The data indicate that fibulins are associated with the hyaluronan-matrix of ECT through a bridge of versican, but that this association changes upon valve development to another supramolecular, presumably microfibrillar organization based on fibronectin and/or fibrillins.

摘要

微原纤维蛋白纤连蛋白-1和纤连蛋白-2先前被鉴定为心脏发育过程中心内膜垫组织(ECT)的主要成分,并显示在成年瓣膜和隔膜中持续存在。免疫金染色现已用于比较它们在胚胎(第9 - 11天)和成年小鼠心脏中的定位与纤连蛋白和硫酸软骨素蛋白聚糖多功能蛋白聚糖的定位。所有这四种蛋白质都沉积在ECT中,ECT由富含透明质酸的、主要无结构的基质组成,但在心肌基底膜或心内膜细胞内几乎检测不到。用透明质酸酶消化可选择性地从ECT中释放纤连蛋白和多功能蛋白聚糖,但不能释放纤连蛋白。然而,与多功能蛋白聚糖相反,在固相分析中两种纤连蛋白都不与透明质酸结合。在成年心脏瓣膜中,所有四种蛋白质都可以在靠近横纹胶原纤维或微原纤维处检测到,但只有多功能蛋白聚糖在暴露于透明质酸酶后会丢失。数据表明,纤连蛋白通过多功能蛋白聚糖桥与ECT的透明质酸基质相关联,但这种关联在瓣膜发育过程中会转变为基于纤连蛋白和/或原纤维蛋白的另一种超分子组织,可能是微原纤维组织。

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