多西环素包裹的纳米管改性牙本质黏结剂。
Doxycycline-encapsulated nanotube-modified dentin adhesives.
作者信息
Feitosa S A, Palasuk J, Kamocki K, Geraldeli S, Gregory R L, Platt J A, Windsor L J, Bottino M C
机构信息
Department of Restorative Dentistry, Division of Dental Biomaterials, Indiana University School of Dentistry, Indianapolis, IN, USA Department of Dental Materials and Prosthodontics, São Paulo State University-UNESP, São José dos Campos, SP, Brazil.
Department of Restorative Dentistry, Division of Dental Biomaterials, Indiana University School of Dentistry, Indianapolis, IN, USA Department of Restorative Dentistry, Faculty of Dentistry, Naresuan University, Phitsanulok, Thailand.
出版信息
J Dent Res. 2014 Dec;93(12):1270-6. doi: 10.1177/0022034514549997. Epub 2014 Sep 8.
This article presents details of fabrication, biological activity (i.e., anti-matrix metalloproteinase [anti-MMP] inhibition), cytocompatibility, and bonding characteristics to dentin of a unique doxycycline (DOX)-encapsulated halloysite nanotube (HNT)-modified adhesive. We tested the hypothesis that the release of DOX from the DOX-encapsulated nanotube-modified adhesive can effectively inhibit MMP activity. We incorporated nanotubes, encapsulated or not with DOX, into the adhesive resin of a commercially available bonding system (Scotchbond Multi-Purpose [SBMP]). The following groups were tested: unmodified SBMP (control), SBMP with nanotubes (HNT), and DOX-encapsulated nanotube-modified adhesive (HNT+DOX). Changes in degree of conversion (DC) and microtensile bond strength were evaluated. Cytotoxicity was examined on human dental pulp stem cells (hDPSCs). To prove the successful encapsulation of DOX within the adhesives-but, more important, to support the hypothesis that the HNT+DOX adhesive would release DOX at subantimicrobial levels-we tested the antimicrobial activity of synthesized adhesives and the DOX-containing eluates against Streptococcus mutans through agar diffusion assays. Anti-MMP properties were assessed via β-casein cleavage assays. Increasing curing times (10, 20, 40 sec) led to increased DC values. There were no statistically significant differences (p > .05) in DC within each increasing curing time between the modified adhesives compared to SBMP. No statistically significant differences in microtensile bond strength were noted. None of the adhesives eluates were cytotoxic to the human dental pulp stem cells. A significant growth inhibition of S. mutans by direct contact illustrates successful encapsulation of DOX into the experimental adhesive. More important, DOX-containing eluates promoted inhibition of MMP-1 activity when compared to the control. Collectively, our findings provide a solid background for further testing of encapsulated MMP inhibitors into the synthesis of therapeutic adhesives that may enhance the longevity of hybrid layers and the overall clinical performance of adhesively bonded resin composite restorations.
本文介绍了一种独特的载多西环素(DOX)的埃洛石纳米管(HNT)改性粘合剂的制备细节、生物活性(即抗基质金属蛋白酶[抗MMP]抑制)、细胞相容性以及与牙本质的粘结特性。我们验证了以下假设:载DOX纳米管改性粘合剂释放的DOX能有效抑制MMP活性。我们将载有或未载DOX的纳米管掺入市售粘结系统(Scotchbond多功能[SBMP])的粘结树脂中。测试了以下几组:未改性的SBMP(对照组)、含纳米管的SBMP(HNT)和载DOX纳米管改性粘合剂(HNT+DOX)。评估了转化率(DC)和微拉伸粘结强度的变化。检测了对人牙髓干细胞(hDPSC)的细胞毒性。为了证明DOX在粘合剂中的成功包封——但更重要的是,为了支持HNT+DOX粘合剂将在亚抗菌水平释放DOX的假设——我们通过琼脂扩散试验测试了合成粘合剂和含DOX洗脱液对变形链球菌的抗菌活性。通过β-酪蛋白裂解试验评估抗MMP特性。固化时间增加(10、20、40秒)导致DC值增加。与SBMP相比,在每个增加的固化时间内,改性粘合剂之间的DC没有统计学显著差异(p>.05)。微拉伸粘结强度没有统计学显著差异。没有一种粘合剂洗脱液对人牙髓干细胞具有细胞毒性。直接接触对变形链球菌有显著的生长抑制作用,说明DOX成功包封在实验粘合剂中。更重要的是,与对照组相比,含DOX的洗脱液促进了MMP-1活性的抑制。总的来说,我们的研究结果为进一步测试包封的MMP抑制剂在治疗性粘合剂合成中的应用提供了坚实的基础,这可能会提高混合层的寿命以及粘结树脂复合材料修复体的整体临床性能。
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