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植入含钛器械的大鼠颅骨时,磷酸化几丁质增加了骨形成。

Phosphorylated chitin increased bone formation when implanted into rat calvaria with the Ti-device.

机构信息

College of Pharmacy and Bioengineering, Chengdu University, Chengdu, Sichuan, China.

Department of Public Health, Matsumoto Dental University, Shiojiri, Japan.

出版信息

Biomed Mater Eng. 2020;31(1):47-57. doi: 10.3233/BME-201079.

Abstract

BACKGROUND

Previously we found that a group of phosphorylated proteins (SIBLINGs) in bone binds with the Ti-device, and increases the early bone formation around the Ti-implants remarkably. From these results, we explained the biochemical mechanism of a strong bond between living bone and Ti, which was discovered by Brånemark and colleagues. For the clinical application of our findings, we need a large amount of these proteins or their substitutes.

OBJECTIVE

We aimed to create a new molecule that equips with essential functions of SIBLINGs, Ti-binding, and bone enhancement around the Ti implant.

METHODS

We chemically phosphorylated chitin and obtained a soluble form of phosphorylated chitin (P-chitin). In this solution, we immersed the Ti-devices of web-form (TW) which we previously developed and obtained the P-chitin coated TWs. Then we tested the P-chitin coated TWs for their calcification ability in vitro, and bone enhancing ability in vivo, by implanting them into rat calvaria. We compared the P-chitin coated TW and the non-coated TW in regard to their calcification and bone enhancing abilities.

RESULTS

Ti-devices coated with phosphorylated-chitin induced a ten times higher calcification in vitro at 20 days, and four times more elevated amount of bone formation in vivo at two weeks than the uncoated Ti-device.

CONCLUSIONS

Phosphorylated chitin could be a partial substitute of bone SIBLING proteins and are clinically applicable to accelerate bone formation around the Ti implants, thereby achieving the strong bond between living bone and Ti.

摘要

背景

此前我们发现,骨中的一组磷酸化蛋白(SIBLINGs)与钛设备结合,并显著增加钛植入物周围的早期骨形成。根据这些结果,我们解释了布伦纳马克和同事发现的活骨与钛之间强结合的生化机制。为了将我们的发现应用于临床,我们需要大量的这些蛋白质或其替代品。

目的

我们旨在创造一种新的分子,它具有 SIBLINGs、与钛结合以及增强钛植入物周围骨的基本功能。

方法

我们对壳聚糖进行化学磷酸化,得到了一种可溶形式的磷酸化壳聚糖(P-壳聚糖)。在这种溶液中,我们将之前开发的网状形式的钛设备(TW)浸入其中,并获得了 P-壳聚糖涂层的 TWs。然后,我们通过将 P-壳聚糖涂层的 TW 植入大鼠颅骨来测试它们在体外的钙化能力和体内的增强骨能力。我们比较了 P-壳聚糖涂层的 TW 和未涂层的 TW 在钙化和增强骨方面的能力。

结果

在 20 天的时间里,用磷酸化壳聚糖涂覆的钛设备在体外诱导的钙化率高 10 倍,在两周内的骨形成量也高 4 倍,高于未涂覆的钛设备。

结论

磷酸化壳聚糖可以作为骨 SIBLING 蛋白的部分替代品,并可临床应用于加速钛植入物周围骨的形成,从而实现活骨与钛之间的牢固结合。

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