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首页> 外文期刊>The Journal of biological chemistry >The Angiogenic Inhibitor Long Pentraxin PTX3 Forms an Asymmetric Octamer with Two Binding Sites for FGF2
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The Angiogenic Inhibitor Long Pentraxin PTX3 Forms an Asymmetric Octamer with Two Binding Sites for FGF2

机译:血管生成抑制剂长五曲素PTX3形成具有两个用于FGF2的两个结合位点的不对称八聚体

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The inflammation-associated long pentraxin PTX3 plays key roles in innate immunity, female fertility, and vascular biology (e.g. it inhibits FGF2 (fibroblast growth factor 2)-mediated angiogenesis). PTX3 is composed of multiple protomers, each composed of distinct N- and C-terminal domains; however, it is not known how these are organized or contribute to its functional properties. Here, biophysical analyses reveal that PTX3 is composed of eight identical protomers, associated through disulfide bonds, forming an elongated and asymmetric, molecule with two differently sized domains interconnected by a stalk. The N-terminal region of the protomer provides the main structural determinant underlying this quaternary organization, supporting formation of a disulfide-linked tetramer and a dimer of dimers (a non-covalent tetramer), giving rise to the asymmetry of the molecule. Furthermore, the PTX3 octamer is shown to contain two FGF2 binding sites, where it is the tetramers that act as the functional units in ligand recognition. Thus, these studies provide a unifying model of the PTX3 oligomer, explaining both its quaternary organization and how this is required for its antiangiogenic function.
机译:炎症相关的长五花素PTX3在先天免疫,女性生育和血管生物学中起关键作用(例如,它抑制FGF2(成纤维细胞生长因子2)介导的血管生成)。 PTX3由多种重选针组成,每个重选式由不同的N-和C末端结构域组成;但是,尚不知道这些是如何组织或有助于其功能性质的。这里,生物物理学分析表明,PTX3由八个相同的重选胶组成,与二硫键相关,形成细长和不对称的分子,其具有由茎互连的两个不同大小的结构域。原子聚物的N末端区域提供了该季度组织的主要结构决定簇,支持形成二硫键连接的四聚物和二聚体(非共价四聚体)的二聚体,从而产生分子的不对称性。此外,PTX3八寡发射机被示出含有两个FGF2结合位点,其中是用作配体识别中的功能单元的四聚体。因此,这些研究提供了PTX3低聚物的统一模型,解释了其第四纪组织以及其抗血管生成功能的方法。

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