研究根管水凝胶的早期顶端释放:一种 3D 打印模型。
Investigation of the early apical release from endodontic hydrogels: A 3D printed model.
机构信息
Laboratoire de Biologie Tissulaire et Ingénierie thérapeutique, UMR 5305 CNRS/Université Claude Bernard Lyon 1, UMS 3444 BioSciences Gerland-Lyon Sud, Lyon, France.
Faculté d'Odontologie, Université Claude Bernard Lyon 1, Université de Lyon, Lyon, France.
出版信息
Int Endod J. 2024 Jul;57(7):943-950. doi: 10.1111/iej.14049. Epub 2024 Feb 20.
AIM
Regenerative Endodontic Procedures (REPs) using new materials such as hydrogels aim to replace current endodontic treatments, but numerous limitations are to overcome. Apical release was little explored in previous studies, especially regarding hydrogels that incorporate molecules, such as growth factors and antibiotics. Apical release is a key mechanism in achieving regeneration, as it could regulate disinfection or cell colonization. Few models exist for apical release, limiting the transfer of these devices from bench to bedside. This study aims to design a simple and standardized model to identify parameters that influence the early apical release kinetic of molecules from endodontic hydrogels.
METHODOLOGY
Endodontic Release Inserts (ERI) were designed to mimic the situation of an immature incisor using three different diameters (Ø 0.5 to 2 mm) and to allow the study of the early release from a hydrogel in a 96-well plate. ERI was produced with a 3D printing machine. The kinetic release was investigated using 2 fluorescent, hydrophobic (BDP-500) and hydrophilic (Fluorescein) molecules, in different hydrogels (fibrin and agarose) and in various media (PBS or serum). The release kinetics were estimated by measuring the fluorescence at different time points (1 to 24 h).
RESULTS
ERI use made it possible to report that apical diameters increase from 500 to 1000 μm was associated with an increase in release from 4.02 ± 1.63% to 11.53 ± 2.38% over 24 h. It also allowed us to report that bottom solution composition change from PBS to human serum was associated with an increase in the release of fatty acid molecules, whilst a decrease in the hydrogel concentration was associated with a variation in release kinetics. Moreover, nano-encapsulation of a molecule was associated with a decreased release over the first 24 h from 5.25 to 0%.
CONCLUSION
ERI use enables investigation of the parameters influencing release kinetics from endodontic hydrogels. Further investigations are necessary to evaluate the interaction of these parameters with each other, in animal models and clinic.
目的
使用水凝胶等新材料的再生牙髓治疗(REP)旨在替代目前的牙髓治疗,但仍有许多局限性需要克服。在之前的研究中,很少探讨根尖释放,特别是涉及到掺入生长因子和抗生素等分子的水凝胶。根尖释放是实现再生的关键机制,因为它可以调节消毒或细胞定植。目前还存在少数用于根尖释放的模型,这限制了这些器械从实验室到临床的转移。本研究旨在设计一种简单且标准化的模型,以确定影响牙髓水凝胶中分子早期根尖释放动力学的参数。
方法
设计了牙髓释放插入物(ERI),以使用三种不同的直径(Ø 0.5 至 2mm)模拟未成熟切牙的情况,并允许在 96 孔板中研究水凝胶的早期释放。ERI 使用 3D 打印机制造。通过荧光(BDP-500 和荧光素)两种疏水性和亲水性分子,在不同的水凝胶(纤维蛋白和琼脂糖)和不同的介质(PBS 或血清)中,研究释放动力学。通过在不同时间点(1 至 24 小时)测量荧光来估计释放动力学。
结果
ERI 的使用使得报告 500 至 1000μm 的根尖直径增加与 24 小时内从 4.02±1.63%增加到 11.53±2.38%的释放相关。它还使我们能够报告底部溶液组成从 PBS 到人血清的变化与脂肪酸分子释放增加相关,而水凝胶浓度降低与释放动力学的变化相关。此外,分子的纳米封装与前 24 小时内的释放减少相关,从 5.25%降至 0%。
结论
ERI 的使用能够研究影响牙髓水凝胶释放动力学的参数。需要进一步研究以评估这些参数彼此之间的相互作用,以及在动物模型和临床中的相互作用。
Zotero 插件