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超分子组装体的底物依赖性形态:原纤维蛋白和VI型胶原微原纤维

Substrate-dependent morphology of supramolecular assemblies: fibrillin and type-VI collagen microfibrils.

作者信息

Sherratt Michael J, Holmes David F, Shuttleworth C Adrian, Kielty Cay M

机构信息

Wellcome Trust Centre for Cell-Matrix Research, School of Biological Sciences, University of Manchester, Manchester, M13 9PT, United Kingdom.

出版信息

Biophys J. 2004 May;86(5):3211-22. doi: 10.1016/S0006-3495(04)74369-6.

Abstract

Substrate hydrophobicity/hydrophilicity has previously been shown to affect the morphology and biological function of isolated proteins. We have employed atomic force microscopy to investigate substrate dependent morphologies of two biochemically distinct native supramolecular assemblies: fibrillin and type-VI collagen microfibrils. These morphologically heterogeneous microfibrillar systems are found in many vertebrate tissues where they perform structural and cell-signaling roles. Fibrillin microfibrils adsorbed to a hydrophilic mica substrate adopted a diffuse morphology. Fibrillin microfibrils adsorbed to mica coated with poly-L-lysine or to borosilicate glass substrates had a more compact morphology and a directional asymmetry to the bead, which was not present on mica alone. Intermediate morphologies were observed along a substrate gradient. The classical double-beaded appearance of type-VI collagen microfibrils was evident on mica coated with poly-L-lysine and on glass. On hydrophilic mica, morphology was severely disrupted and there was a major conformational reorganization along the whole collagen microfibril repeat. These observations of substrate dependent conformation have important implications for the interpretation of data from in vitro protein interaction assays and cellular signaling studies. Furthermore, conformational changes may be induced by local charge environments in vivo, revealing or hiding binding sites.

摘要

底物的疏水性/亲水性此前已被证明会影响分离蛋白质的形态和生物学功能。我们利用原子力显微镜研究了两种生化性质不同的天然超分子组装体——原纤维蛋白和VI型胶原微纤维——的底物依赖性形态。这些形态各异的微纤维系统存在于许多脊椎动物组织中,在其中发挥结构和细胞信号传导作用。吸附在亲水性云母底物上的原纤维蛋白微纤维呈现出弥散的形态。吸附在涂有聚-L-赖氨酸的云母或硼硅酸盐玻璃底物上的原纤维蛋白微纤维具有更紧密的形态,并且对珠子有方向不对称性,而单独的云母上不存在这种情况。沿着底物梯度观察到了中间形态。VI型胶原微纤维的经典双珠外观在涂有聚-L-赖氨酸的云母和玻璃上很明显。在亲水性云母上,形态严重破坏,并且沿着整个胶原微纤维重复单元发生了主要的构象重组。这些关于底物依赖性构象的观察结果对于解释体外蛋白质相互作用测定和细胞信号传导研究的数据具有重要意义。此外,体内局部电荷环境可能会诱导构象变化,从而暴露或隐藏结合位点。

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