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桥粒芯糖蛋白特异性胞质区域在溶液中本质上是无序的,并且与多种桥粒蛋白伙伴相互作用。

The desmoglein-specific cytoplasmic region is intrinsically disordered in solution and interacts with multiple desmosomal protein partners.

作者信息

Kami Keiichiro, Chidgey Martyn, Dafforn Timothy, Overduin Michael

机构信息

University of Birmingham, UK.

出版信息

J Mol Biol. 2009 Feb 20;386(2):531-43. doi: 10.1016/j.jmb.2008.12.054. Epub 2008 Dec 30.

DOI:10.1016/j.jmb.2008.12.054
PMID:19136012
Abstract

The desmoglein-specific cytoplasmic region (DSCR) is a conserved region of unknown structure and function that uniquely defines the desmoglein family of cell adhesion molecules. It is the site of caspase cleavage during apoptosis, and its mutation is linked to cardiomyopathy. Here, we reveal that a 276-residue DSCR construct of human desmoglein 1 is intrinsically disordered and forms an interaction hub for desmosomal proteins. In solution, it contains 6.5% helical and 10.3% beta-strand structure based on circular dichroism spectroscopy. A single monomeric state with a predominantly unfolded structure is found by size-exclusion chromatography and analytical ultracentrifugation. Thermal stability assays and nuclear magnetic resonance spectroscopy reveal a nonglobular structure under a range of solution conditions. However, the introduction of detergent micelles increases structure to 18% helical and 16% beta-strand character, suggesting an inducible structure. The DSCR exhibits weak but specific interactions with plakoglobin, the plakin domain of desmoplakin, plakophilin 1, and the cytoplasmic domain of desmocollin 1. The desmoglein 1 membrane proximal region also interacts with all four DSCR ligands, strongly with plakoglobin and plakophilin and more weakly with desmoplakin and desmocollin 1. Thus, the DSCR is an intrinsically disordered functional domain with an inducible structure that, along with the membrane proximal region, forms a flexible scaffold for cytoplasmic assembly at the desmosome.

摘要

桥粒芯糖蛋白特异性胞质区域(DSCR)是一个结构和功能未知的保守区域,它独特地定义了细胞粘附分子的桥粒芯糖蛋白家族。它是细胞凋亡过程中半胱天冬酶切割的位点,其突变与心肌病有关。在这里,我们揭示了人桥粒芯糖蛋白1的一个由276个残基组成的DSCR构建体本质上是无序的,并且形成了一个桥粒蛋白的相互作用中心。在溶液中,根据圆二色光谱,它含有6.5%的螺旋结构和10.3%的β链结构。通过尺寸排阻色谱和分析超速离心发现其处于主要为未折叠结构的单一单体状态。热稳定性分析和核磁共振光谱显示在一系列溶液条件下其结构是非球状的。然而,引入去污剂胶束会使结构增加到18%的螺旋结构和16%的β链结构特征,表明其具有可诱导结构。DSCR与桥粒斑珠蛋白、桥粒斑蛋白的斑珠蛋白结构域、桥粒芯蛋白1和桥粒胶蛋白1的胞质结构域表现出微弱但特异的相互作用。桥粒芯糖蛋白1膜近端区域也与所有四种DSCR配体相互作用,与桥粒斑珠蛋白和桥粒芯蛋白强烈相互作用,与桥粒斑蛋白和桥粒胶蛋白1相互作用较弱。因此,DSCR是一个具有可诱导结构的本质上无序的功能结构域,它与膜近端区域一起,在桥粒处形成了一个用于细胞质组装的灵活支架。

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