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原纤蛋白-1的纳米结构揭示了表皮生长因子阵列的紧密构象及可伸展性机制。

Nanostructure of fibrillin-1 reveals compact conformation of EGF arrays and mechanism for extensibility.

作者信息

Baldock Clair, Siegler Veronique, Bax Daniel V, Cain Stuart A, Mellody Kieran T, Marson Andrew, Haston J Louise, Berry Richard, Wang Ming-Chuan, Grossmann J Günter, Roessle Manfred, Kielty Cay M, Wess Tim J

机构信息

Wellcome Trust Centre for Cell-Matrix Research, Faculty of Life Sciences, Michael Smith Building, University of Manchester, Greater Manchester M13 9PT, UK.

出版信息

Proc Natl Acad Sci U S A. 2006 Aug 8;103(32):11922-7. doi: 10.1073/pnas.0601609103. Epub 2006 Jul 31.

Abstract

Fibrillin-1 is a 330-kDa multidomain extracellular matrix protein that polymerizes to form 57-nm periodic microfibrils, which are essential for all tissue elasticity. Fibrillin-1 is a member of the calcium-binding EGF repeat family and has served as a prototype for structural analyses. Nevertheless, both the detailed structure of fibrillin-1 and its organization within microfibrils are poorly understood because of the complexity of the molecule and the resistance of EGF arrays to crystallization. Here, we have used small-angle x-ray scattering and light scattering to analyze the solution structure of human fibrillin-1 and to produce ab initio structures of overlapping fragments covering 90% of the molecule. Rather than exhibiting a uniform rod shape as current models predict, the scattering data revealed a nonlinear conformation of calcium-binding EGF arrays in solution. This finding has major implications for the structures of the many other EGF-containing extracellular matrix and membrane proteins. The scattering data also highlighted a very compact, globular region of the fibrillin-1 molecule, which contains the integrin and heparan sulfate-binding sites. This finding was confirmed by calculating a 3D reconstruction of this region using electron microscopy and single-particle image analysis. Together, these data have enabled the generation of an improved model for microfibril organization and a previously undescribed mechanism for microfibril extensibility.

摘要

原纤蛋白-1是一种330千道尔顿的多结构域细胞外基质蛋白,它聚合形成57纳米周期性微原纤维,这对所有组织的弹性至关重要。原纤蛋白-1是钙结合表皮生长因子重复序列家族的成员,并且已成为结构分析的原型。然而,由于该分子的复杂性以及表皮生长因子阵列难以结晶,原纤蛋白-1的详细结构及其在微原纤维中的组织形式仍知之甚少。在这里,我们利用小角X射线散射和光散射来分析人原纤蛋白-1的溶液结构,并生成覆盖该分子90%的重叠片段的从头算结构。散射数据显示,溶液中的钙结合表皮生长因子阵列呈现非线性构象,而不是像当前模型所预测的那样呈现均匀的杆状。这一发现对许多其他含表皮生长因子的细胞外基质和膜蛋白的结构具有重要意义。散射数据还突出显示了原纤蛋白-1分子中一个非常紧凑的球状区域,该区域包含整合素和硫酸乙酰肝素结合位点。通过使用电子显微镜和单颗粒图像分析计算该区域的三维重建,这一发现得到了证实。总之,这些数据使得能够生成一个改进的微原纤维组织模型和一种以前未描述的微原纤维可扩展性机制。

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