NAPROXEN/LAYERED DOUBLE HYDROXIDE COMPOSITES FOR TISSUE-ENGINEERING APPLICATIONS: PHYSICOCHEMICAL CHARACTERIZATION AND BIOLOGICAL EVALUATION

被引:0
|
作者
Marcela P. Bernardo
Bruna C.S. Rodrigues
Tamires D. de Oliveira
Adriana P.M. Guedes
Alzir A. Batista
Luiz H.C. Mattoso
机构
[1] Brazilian Agricultural Research Corporation,National Nanotechnology Laboratory for Agribusiness, Embrapa Instrumentation
[2] Federal University of São Carlos,Department of Chemistry
来源
Clays and Clay Minerals | 2020年 / 68卷
关键词
Biomaterials; Controlled release; Cytotoxicity; Hydrotalcite; NSAID; Structural reconstruction;
D O I
暂无
中图分类号
学科分类号
摘要
Injured bone tissues can be healed with bone grafts, but this procedure may cause intense pain to the patient. A slow and localized delivery of nonsteroidal anti-inflammatory drugs (NSAIDs) could help to reduce the pain without affecting bone regeneration. The objective of the present study was to use [Mg-Al]-layered double hydroxide (LDH) as a matrix for controlled release of sodium naproxen (NAP). This system could be applied in biomaterial formulations (such as bone grafts) to achieve a local delivery of naproxen. [Mg-Al]-LDH successfully incorporated up to 80% (w/w) of naproxen by the structural reconstruction route, with the [Mg-Al]-LDH interlayer space increasing by 0.55 nm, corresponding to the drug molecule size. The evaluation of the naproxen release kinetics showed that 40% of the drug was delivered over 48 h in aqueous medium (pH 7.4 ± 0.1), indicating the potential of [Mg-Al]-LDH/NAP for local release of naproxen at adequate concentrations. Kinetic modeling showed that the naproxen release process was closely related to the Higuchi model, which considers the drug release as a diffusional process based on Fick’s law. The chemical stability of NAP after the release tests was verified by 1H NMR. The [Mg-Al]-LDH/NAP also exhibited low cytotoxicity toward fibroblast cells (L929 cell line), without modifications in their morphology and adhesion capacity. These results describe a suitable approach for preparing efficient systems for local delivery of nonsteroidal anti-inflammatory drugs for biomedical applications.
引用
收藏
页码:623 / 631
页数:8
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