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基于纳米黏土的透皮给药复合膜:开发、表征以及计算机建模与模拟。

Nanoclay-Based Composite Films for Transdermal Drug Delivery: Development, Characterization, and in silico Modeling and Simulation.

机构信息

Department of Pharmaceutics, Faculty of Pharmacy and Pharmaceutical Sciences, University of Karachi, Karachi, 75270, Pakistan.

Jinnah College of Pharmacy, Sohail University, Karachi, 74000, Pakistan.

出版信息

Int J Nanomedicine. 2022 Aug 4;17:3463-3481. doi: 10.2147/IJN.S367540. eCollection 2022.

Abstract

PURPOSE

Halloysite nanotubes (HNTs) are a versatile and highly investigated clay mineral due to their natural availability, low cost, strong mechanical strength, biocompatibility, and binding properties. The present work explores its role for retarding and controlling the drug release from the composite polymer matrix material.

METHODS

For this purpose, nanocomposite films comprising propranolol HCl and different concentrations of HNTs were formulated using the "solution casting method". The menthol in a concentration of 1% w/v was used as a permeation enhancer, and its effect on release and permeation was also determined. Quality characteristics of the nanocomposite were determined, and in vitro release and permeation studies were performed using the Franz diffusion system. The data was analyzed using various mathematical models and permeation parameters. Optimized formulation was also subjected to skin irritation test, FTIR, DSC, and SEM study. Systemic absorption and disposition of propranolol HCl from the nanocomposites were predicted using the GastroPlus TCAT® model.

RESULTS

The control in drug release rate was associated with the higher concentration of HNTs. F8 released 50% of propranolol within 8 hours (drug, HNTs ratio, 1:2). The optimized formulation (F6) with drug: HNTs (2:1), exhibited drug release 80% in 4 hours, with maximum flux of 145.812 µg/cmhr. The optimized formulation was found to be a non-irritant for skin with a shelf life of 35.46 months (28-30 ℃). The in silico model predicted , and as 32.113 ng/mL, 16.58 h, 942.34 ng/mL×h, and 1102.9 ng/mL×h, respectively.

CONCLUSION

The study demonstrated that HNTs could be effectively used as rate controlling agent in matrix type transdermal formulations.

摘要

目的

由于海泡石纳米管(HNTs)具有天然可用性、低成本、高强度、生物相容性和结合特性,因此它是一种多功能且经过深入研究的粘土矿物。本研究探讨了其在控制药物从复合聚合物基质材料中释放的作用。

方法

为此,采用“溶液浇铸法”制备了包含盐酸普萘洛尔和不同浓度 HNTs 的纳米复合膜。以 1%(w/v)浓度的薄荷醇作为渗透增强剂,并确定其对释放和渗透的影响。测定纳米复合材料的质量特性,并使用 Franz 扩散系统进行体外释放和渗透研究。使用各种数学模型和渗透参数对数据进行分析。还对优化的配方进行了皮肤刺激性试验、FTIR、DSC 和 SEM 研究。使用 GastroPlus TCAT®模型预测了盐酸普萘洛尔从纳米复合材料中的系统吸收和处置。

结果

控制药物释放速率与 HNTs 的浓度较高有关。F8 在 8 小时内释放了 50%的盐酸普萘洛尔(药物:HNTs 比例为 1:2)。药物:HNTs(2:1)的优化配方(F6)在 4 小时内释放了 80%的药物,最大通量为 145.812µg/cmhr。优化的配方对皮肤无刺激性,保质期为 35.46 个月(28-30℃)。体内模型预测 、 、 分别为 32.113ng/mL、16.58h、942.34ng/mL×h 和 1102.9ng/mL×h。

结论

研究表明,HNTs 可有效用作基质型透皮制剂的控释剂。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1392/9359522/5fc91cb915a9/IJN-17-3463-g0001.jpg

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