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酶促、尿素酶介导的碳酸钙、富镁碳酸钙和碳酸镁对结冷胶水凝胶的矿化作用及其在骨再生中的应用。

Enzymatic, urease-mediated mineralization of gellan gum hydrogel with calcium carbonate, magnesium-enriched calcium carbonate and magnesium carbonate for bone regeneration applications.

机构信息

Department Molecular Biotechnology, Ghent University, Belgium.

Department of Biomaterials, Faculty of Materials Science and Ceramics, AGH University of Science and Technology, Kraków, Poland.

出版信息

J Tissue Eng Regen Med. 2017 Dec;11(12):3556-3566. doi: 10.1002/term.2273. Epub 2017 Jun 1.

Abstract

Mineralization of hydrogel biomaterials is considered desirable to improve their suitability as materials for bone regeneration. Calcium carbonate (CaCO ) has been successfully applied as a bone regeneration material, but hydrogel-CaCO composites have received less attention. Magnesium (Mg) has been used as a component of calcium phosphate biomaterials to stimulate bone-forming cell adhesion and proliferation and bone regeneration in vivo, but its effect as a component of carbonate-based biomaterials remains uninvestigated. In the present study, gellan gum (GG) hydrogels were mineralized enzymatically with CaCO , Mg-enriched CaCO and magnesium carbonate to generate composite biomaterials for bone regeneration. Hydrogels loaded with the enzyme urease were mineralized by incubation in mineralization media containing urea and different ratios of calcium and magnesium ions. Increasing the magnesium concentration decreased mineral crystallinity. At low magnesium concentrations calcite was formed, while at higher concentrations magnesian calcite was formed. Hydromagnesite (Mg (CO ) (OH) .4H O) formed at high magnesium concentration in the absence of calcium. The amount of mineral formed and compressive strength decreased with increasing magnesium concentration in the mineralization medium. The calcium:magnesium elemental ratio in the mineral formed was higher than in the respective mineralization media. Mineralization of hydrogels with calcite or magnesian calcite promoted adhesion and growth of osteoblast-like cells. Hydrogels mineralized with hydromagnesite displayed higher cytotoxicity. In conclusion, enzymatic mineralization of GG hydrogels with CaCO in the form of calcite successfully reinforced hydrogels and promoted osteoblast-like cell adhesion and growth, but magnesium enrichment had no definitive positive effect. Copyright © 2017 John Wiley & Sons, Ltd.

摘要

水凝胶生物材料的矿化被认为是提高其作为骨再生材料适用性的理想方法。碳酸钙 (CaCO ) 已成功应用于骨再生材料,但水凝胶-CaCO 复合材料的关注度较低。镁 (Mg) 已被用作磷酸钙生物材料的组成部分,以刺激成骨细胞的黏附和增殖以及体内的骨再生,但它作为基于碳酸盐的生物材料的组成部分的作用尚未得到研究。在本研究中,用 CaCO 、富含镁的 CaCO 和碳酸镁酶促矿化结冷胶 (GG) 水凝胶,生成用于骨再生的复合生物材料。用脲酶负载的水凝胶在含有尿素和不同钙镁离子比例的矿化介质中孵育,进行矿化。增加镁浓度会降低矿物结晶度。在低镁浓度下形成方解石,而在较高浓度下形成镁方解石。在没有钙的情况下,高镁浓度下形成水菱镁矿 (Mg (CO ) (OH).4H O)。随着矿化介质中镁浓度的增加,形成的矿物量和抗压强度降低。形成的矿物中钙与镁的元素比高于相应的矿化介质。用方解石或镁方解石矿化水凝胶促进成骨样细胞的黏附和生长。用水菱镁矿矿化的水凝胶显示出更高的细胞毒性。总之,用 CaCO 形式的方解石对 GG 水凝胶进行酶促矿化成功地增强了水凝胶,并促进了成骨样细胞的黏附和生长,但镁的富集没有明确的积极作用。版权所有 © 2017 约翰威立父子公司

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