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用于经颊麻醉的纳米杂化水凝胶。

Nanohybrid hydrogels designed for transbuccal anesthesia.

机构信息

Department of Biochemistry and Tissue Biology, Institute of Biology, University of Campinas (Unicamp), Campinas, São Paulo, Brazil,

Department of Physiological Sciences, Piracicaba Dental School, Unicamp, Piracicaba, São Paulo, Brazil.

出版信息

Int J Nanomedicine. 2018 Oct 15;13:6453-6463. doi: 10.2147/IJN.S180080. eCollection 2018.

Abstract

BACKGROUND

Local anesthesia in dentistry is by far the most terrifying procedure for patients, causing treatment interruption. None of the commercially available topical formulations is effective in eliminating the pain and phobia associated to the needle insertion and injection.

MATERIALS AND METHODS

In this work we prepared a nanostructured lipid-biopolymer hydrogel for the sustained delivery of lidocaine-prilocaine (LDC-PLC) for transbuccal pre-anesthesia. The lipid was composed of optimized nanostructured lipid carriers (NLC) loaded with 5% LDC-PLC (NLC/LDC-PLC). The biopolymer counterpart was selected among alginate, xanthan (XAN), and chitosan matrices. The XAN-NLC hydrogel presented the most uniform aspect and pseudoplastic rheological profile, as required for topical use; therefore, it was selected for subsequent analyses. Accelerated stability tests under critical conditions (40°C; 75% relative humidity) were conducted for 6 months, in terms of drug content (mg/g), weight loss (%), and pH.

RESULTS

In vitro LDC-PLC release profile through Franz diffusion cells revealed a bimodal kinetics with a burst effect followed by the sustained release of both anesthetics, for 24 hours. Structural analyses (fourier transform infrared spectroscopy, differential scanning calorimetry and scanning electron microscopy) gave details on the molecular organization of the hybrid hydrogel, confirming the synergic interaction between the components. Safety and efficacy were evaluated through in vitro cell viability (3T3, HaCat, and VERO cells) and in vivo antinociceptive (tail-flick, in mice) tests, respectively. In comparison to a control hydrogel and the eutectic mixture of 5% LDC-PLC cream (EMLA), the XAN-NLC/LDC-PLC hybrid hydrogel doubled and quadrupled the anesthetic effect (8 hours), respectively.

CONCLUSION

Considering such exciting results, this multifaceted nanohybrid system is now ready to be further tested in clinical trials.

摘要

背景

在牙科中,局部麻醉迄今为止是患者最害怕的治疗程序,会导致治疗中断。目前市售的任何一种局部制剂都不能有效消除与针插入和注射相关的疼痛和恐惧。

材料和方法

在这项工作中,我们为经颊部预麻醉制备了一种用于持续输送利多卡因-丙胺卡因(LDC-PLC)的纳米结构化脂质-生物聚合物水凝胶。脂质由负载 5% LDC-PLC 的优化纳米结构化脂质载体(NLC)组成(NLC/LDC-PLC)。生物聚合物则在藻酸盐、黄原胶(XAN)和壳聚糖基质中进行选择。XAN-NLC 水凝胶具有最均匀的外观和假塑性流变特性,符合局部使用的要求;因此,它被选为后续分析。在关键条件(40°C;75%相对湿度)下进行了 6 个月的加速稳定性测试,包括药物含量(mg/g)、失重(%)和 pH 值。

结果

通过 Franz 扩散细胞进行的体外 LDC-PLC 释放曲线显示出双模式动力学,具有爆发效应,随后两种麻醉剂持续释放 24 小时。结构分析(傅里叶变换红外光谱、差示扫描量热法和扫描电子显微镜)详细说明了混合水凝胶的分子组织,证实了各成分之间的协同相互作用。通过体外细胞活力(3T3、HaCat 和 VERO 细胞)和体内镇痛(小鼠尾部闪烁)测试分别评估了安全性和功效。与对照水凝胶和 5% LDC-PLC 乳膏的共晶混合物(EMLA)相比,XAN-NLC/LDC-PLC 杂化水凝胶分别将麻醉效果提高了一倍和四倍(8 小时)。

结论

考虑到这些令人兴奋的结果,这种多功能纳米杂化系统现在已准备好进一步进行临床试验。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5d57/6198882/8ae63828e954/ijn-13-6453Fig1.jpg

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