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无序构象与低 Pii 螺旋的磷蛋白协调仿生磷灰石的形成。

Disordered Conformation with Low Pii Helix in Phosphoproteins Orchestrates Biomimetic Apatite Formation.

机构信息

Institute for Macromolecular Chemistry, BIOSS Centre for Biological Signaling Studies, University of Freiburg, 79104, Freiburg, Germany.

Helmholtz Virtual Institute, Multifunctional Biomaterials for Medicine, Kantstr. 55, 14513, Teltow, Germany.

出版信息

Adv Mater. 2017 Sep;29(35). doi: 10.1002/adma.201701629. Epub 2017 Jul 17.

Abstract

The interplay between noncollagenous proteins and biomineralization is widely accepted, yet the contribution of their secondary structure in mineral formation remains to be clarified. This study demonstrates a role for phosvitin, an intrinsically disordered phosphoprotein, in chick embryo skeletal development, and using circular dichroism and matrix least-squares Henderson-Hasselbalch global fitting, unravels three distinct pH-dependent secondary structures in phosvitin. By sequestering phosvitin on a biomimetic 3D insoluble cationic framework at defined pHs, access is gained to phosvitin in various conformational states. Induction of biomimetic mineralization at near physiological conditions reveals that a disordered secondary structure with a low content of P helix is remarkably efficient at promoting calcium adsorption, and results in the formation of biomimetic hydroxyapatite through an amorphous calcium phosphate precursor. By extending this finding to phosphorylated full-length human recombinant dentin matrix protein-1 (17-513 AA), this bioinspired approach provides compelling evidence for the role of a disordered secondary structure in phosphoproteins in bone-like apatite formation.

摘要

非胶原蛋白和生物矿化之间的相互作用是被广泛接受的,然而它们的二级结构在矿物形成中的作用仍有待阐明。本研究表明,磷酸化蛋白卵黄高磷蛋白在鸡胚骨骼发育中起作用,并通过圆二色性和矩阵最小二乘法 Henderson-Hasselbalch 全局拟合,揭示了卵黄高磷蛋白中三种不同的 pH 依赖性二级结构。通过在特定 pH 值下将卵黄高磷蛋白固定在仿生 3D 不溶性阳离子骨架上,可以获得处于各种构象状态的卵黄高磷蛋白。在接近生理条件下诱导仿生矿化表明,具有低 P 螺旋含量的无序二级结构在促进钙吸附方面非常有效,并通过无定形磷酸钙前体形成仿生羟基磷灰石。通过将这一发现扩展到磷酸化全长人重组牙本质基质蛋白-1(17-513AA),这种受生物启发的方法为磷酸化蛋白在类骨磷灰石形成中的无序二级结构的作用提供了有力的证据。

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