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通过类淀粉样牙釉原蛋白模拟物控制釉质再矿化。

Controlling Enamel Remineralization by Amyloid-Like Amelogenin Mimics.

机构信息

School of Mechanical and Precision Instrument Engineering, Xi'an University of Technology, Xi'an, 710048, China.

School and Hospital of Stomatology, Tianjin Medical University, 12 Observatory Road, Tianjin, 30070, China.

出版信息

Adv Mater. 2020 Aug;32(31):e2002080. doi: 10.1002/adma.202002080. Epub 2020 Jun 25.

DOI:10.1002/adma.202002080
PMID:32583928
Abstract

In situ regeneration of the enamel-like structure of hydroxyapatite (HAp) crystals under oral conditions is significant for dental caries treatment. However, it is still a challenge for dentists to duplicate the elegant and well-aligned apatite structure bonding to the surface of demineralized enamel. A biocompatible amelogenin-inspired matrix, a phase-transited lysozyme (PTL) film mimicking an N-terminal amelogenin with central domain (N-Ame) combined with synthetic peptide (C-AMG) based on the functional domains of C-terminal telopeptide (C-Ame) is shown here, which is formed by amyloid-like lysozyme aggregation at the enamel interface through a rapid one-step aqueous coating process. In the PTL/C-AMG matrix, C-AMG facilitated the oriented arrangement of amorphous calcium phosphate (ACP) nanoparticles and their transformation to ordered enamel-like HAp crystals, while PTL served as a strong interfacial anchor to immobilize the C-AMG peptide and PTL/C-AMG matrix on versatile substrate surfaces. PTL/C-AMG film-coated enamel induced both of the in vivo and in vitro synthesis of HAp crystals, facilitated epitaxial growth of HAp crystals and recovered the highly oriented structure and mechanical properties to levels nearly identical to those of natural enamel. This work underlines the importance of amyloid-like protein aggregates in the biomineralization of enamel, providing a promising strategy for treating dental caries.

摘要

在口腔环境下原位再生羟磷灰石(HAp)晶体的类釉质结构对于龋齿治疗具有重要意义。然而,对于牙医来说,复制与脱矿釉质表面结合的优雅且排列整齐的磷灰石结构仍然是一个挑战。在这里,展示了一种生物相容性的釉原蛋白模拟基质,即通过在釉质界面上通过快速的一步水包衣过程形成的类淀粉样溶菌酶(PTL)薄膜,模拟具有中央结构域的 N 端釉原蛋白(N-Ame)与基于 C 端末端肽(C-Ame)的功能域的合成肽(C-AMG)结合。在 PTL/C-AMG 基质中,C-AMG 促进了无定形磷酸钙(ACP)纳米颗粒的有序排列及其向有序类釉质 HAp 晶体的转化,而 PTL 则作为强界面锚定物将 C-AMG 肽和 PTL/C-AMG 基质固定在多种基底表面上。PTL/C-AMG 薄膜涂层牙釉质可诱导体内和体外 HAp 晶体的合成,促进 HAp 晶体的外延生长,并恢复高度有序的结构和机械性能,使其接近天然牙釉质的水平。这项工作强调了类淀粉样蛋白聚集体在牙釉质生物矿化中的重要性,为治疗龋齿提供了一种有前途的策略。

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