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介导自身相互作用的层粘连蛋白N端结构域的分子分析。

Molecular analysis of laminin N-terminal domains mediating self-interactions.

作者信息

Odenthal Uwe, Haehn Sebastian, Tunggal Patrick, Merkl Barbara, Schomburg Dietmar, Frie Christian, Paulsson Mats, Smyth Neil

机构信息

Center for Biochemistry and Center for Molecular Medicine, Faculty of Medicine, University of Cologne, Joseph-Stelzmann-Strasse 52, Cologne D-50931, Germany.

出版信息

J Biol Chem. 2004 Oct 22;279(43):44504-12. doi: 10.1074/jbc.M402455200. Epub 2004 Aug 13.

DOI:10.1074/jbc.M402455200
PMID:15310759
Abstract

The ability of laminins to self-polymerize is crucial for the formation of basement membranes. Development of this polymerized network has profound effects upon tissue architecture as well as on the intracellular organization and differentiation of neighboring cells. The laminin N-terminal (LN) domains have been shown to mediate this interaction and studies using proteolytic fragments derived from laminin-1 led to the theory that network assembly depends on the formation of a heterotrimeric complex between LN domains derived from alpha, beta, and gamma chains in different laminin molecules with homologous interactions being insignificant. The laminin family consists of 15 known isoforms formed from five alpha, three beta, and three gamma chains, of which some are truncated and lack the N-terminal LN domain. To address whether the model of heterotrimeric complex formation is applicable to laminin isoforms other than laminin-1, eight LN domains found in the laminin protein family were recombinantly expressed and tested in three different assays for homologous and heterologous interactions. The results showed that the lack of homologous interactions is an exception, with such interactions being seen for LN domains derived from all alpha chains and from the beta2 and beta3 subunits. The gamma chain-derived LN domains showed a far more limited binding repertoire, particularly in the case of the gamma3 chain, which is found present in a range of non-basement membrane locations. Further, whereas the interactions depended upon Ca2+ ions, with EDTA reversibly abrogating binding, EDTA-induced conformational changes were not reversible. Together these results demonstrate that the assembly model proposed on the basis of laminin-1 may be a simplification, with the assembly of naturally occurring laminin networks being far more complex and highly dependent upon which laminin isoforms are present.

摘要

层粘连蛋白自我聚合的能力对于基底膜的形成至关重要。这种聚合网络的形成对组织结构以及相邻细胞的细胞内组织和分化具有深远影响。层粘连蛋白N端(LN)结构域已被证明可介导这种相互作用,使用源自层粘连蛋白-1的蛋白水解片段进行的研究得出了这样的理论,即网络组装依赖于不同层粘连蛋白分子中源自α、β和γ链的LN结构域之间形成异源三聚体复合物,同源相互作用并不重要。层粘连蛋白家族由15种已知的异构体组成,这些异构体由5条α链、3条β链和3条γ链形成,其中一些是截短的,缺乏N端LN结构域。为了探究异源三聚体复合物形成模型是否适用于层粘连蛋白-1以外的层粘连蛋白异构体,在层粘连蛋白蛋白家族中发现的8个LN结构域被重组表达,并在三种不同的试验中测试同源和异源相互作用。结果表明,缺乏同源相互作用是个例外,所有α链以及β2和β3亚基的LN结构域都存在这种相互作用。γ链衍生的LN结构域显示出更有限的结合谱,特别是γ3链的情况,它存在于一系列非基底膜位置。此外,虽然相互作用依赖于Ca2+离子,EDTA可逆转地消除结合,但EDTA诱导的构象变化是不可逆的。这些结果共同表明,基于层粘连蛋白-1提出的组装模型可能过于简化,天然存在的层粘连蛋白网络的组装要复杂得多,并且高度依赖于存在哪些层粘连蛋白异构体。

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