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以铜/抗坏血酸络合物为前驱体合成高铜浓度的高度分散介孔生物活性玻璃纳米颗粒

Toward Highly Dispersed Mesoporous Bioactive Glass Nanoparticles With High Cu Concentration Using Cu/Ascorbic Acid Complex as Precursor.

作者信息

Zheng Kai, Kang Jeonil, Rutkowski Bogdan, Gawȩda Magdalena, Zhang Jue, Wang You, Founier Niklas, Sitarz Maciej, Taccardi Nicola, Boccaccini Aldo R

机构信息

Institute of Biomaterials, University of Erlangen-Nuremberg, Erlangen, Germany.

Faculty of Metals Engineering and Industrial Computer Science, AGH University of Science and Technology, Kraków, Poland.

出版信息

Front Chem. 2019 Jul 16;7:497. doi: 10.3389/fchem.2019.00497. eCollection 2019.

Abstract

Copper (Cu) ions have a variety of advantageous biological functionalities, such as proangiogenic and bactericidal activities. Given the intrinsic biodegradability and biocompatibility, silicate-based mesoporous bioactive glass nanoparticles (MBGNs) are considered as promising platforms for the delivery of Cu ions. However, effective incorporation of Cu into MBGNs still faces challenges, e.g., particle aggregation, the formation of insoluble crystalline Cu-based nanoparticles, and a low loading amount of Cu. We report a novel method to synthesize chemically homogenous and highly dispersed Cu-containing MBGNs (Cu-MBGNs) with tunable Cu concentration by using ascorbic acid/Cu complexes as the precursor of Cu in a microemulsion-assisted sol-gel approach. Cu-MBGNs exhibited a sphere-like shape with a particle size between 100 and 300 nm while their pore size varied from 2 to 10 nm. The inclusion of Cu, regardless of the incorporated concentration, did not significantly affect the morphology of particles. ICP-AES results indicated that the concentration of Cu in the particles could be conveniently tuned from 0 to ~6 mol% by controlling the amount of ascorbic acid/Cu complexes added, while the formation of crystalline Cu-based nanoparticles was avoided. The amorphous feature of Cu-MBGNs was proved by XRD, while the predominant oxidation state of Cu was evidenced to be Cu by XPS. The incorporation of Cu did not inhibit the apatite-forming ability (bioactivity) of the particles in contact with simulated body fluid. Cu-MBGNs exhibited the capability of releasing Cu, Si, and Ca ions over time in the physiological fluid. The concentration of released Cu ions could be controlled by selecting specific Cu-MBGNs of different Cu contents. The dissolution products of most Cu-MBGNs at the dosage of 1, 0.1, and 0.01 mg/mL did not exhibit cytotoxicity, while only 7Cu-MBGN was cytotoxic at the dosage of 1 mg/mL. This study provided a feasible strategy to synthesize highly dispersed amorphous Cu-MBGNs with high Cu concentrations for biomedical applications. The particles exhibit great potential as building blocks for developing composite 3D scaffolds, coatings, and drug carriers, particularly when a large amount of particles incorporated may compromise the properties of (polymer) matrix materials while a relatively high concentration of released Cu ions is still required.

摘要

铜(Cu)离子具有多种有益的生物功能,如促血管生成和杀菌活性。鉴于其固有的生物可降解性和生物相容性,基于硅酸盐的介孔生物活性玻璃纳米颗粒(MBGNs)被认为是递送铜离子的有前景的平台。然而,将铜有效地掺入MBGNs仍面临挑战,例如颗粒聚集、不溶性结晶铜基纳米颗粒的形成以及铜的低负载量。我们报道了一种新方法,通过在微乳液辅助溶胶 - 凝胶法中使用抗坏血酸/Cu络合物作为铜的前体,合成具有可调铜浓度的化学均匀且高度分散的含铜MBGNs(Cu-MBGNs)。Cu-MBGNs呈球形,粒径在100至300nm之间,而其孔径在2至10nm之间变化。铜的掺入,无论其掺入浓度如何,均未显著影响颗粒的形态。电感耦合等离子体原子发射光谱(ICP-AES)结果表明,通过控制抗坏血酸/Cu络合物的添加量,颗粒中铜的浓度可方便地从0调整到约6mol%,同时避免了结晶铜基纳米颗粒的形成。XRD证明了Cu-MBGNs的非晶态特征,而XPS表明铜的主要氧化态为Cu。铜的掺入并未抑制颗粒与模拟体液接触时的磷灰石形成能力(生物活性)。Cu-MBGNs在生理流体中表现出随时间释放铜、硅和钙离子的能力。释放的铜离子浓度可通过选择不同铜含量的特定Cu-MBGNs来控制。大多数Cu-MBGNs在1mg/mL、0.1mg/mL和0.01mg/mL剂量下的溶解产物未表现出细胞毒性,而只有7Cu-MBGN在1mg/mL剂量下具有细胞毒性。本研究提供了一种可行的策略,用于合成用于生物医学应用的具有高铜浓度的高度分散的非晶态Cu-MBGNs。这些颗粒作为开发复合3D支架、涂层和药物载体的构建单元具有巨大潜力,特别是当大量掺入颗粒可能损害(聚合物)基体材料的性能而仍需要相对高浓度的释放铜离子时。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ecff/6646719/05dfb386e771/fchem-07-00497-g0001.jpg

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