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Soluplus 胶束用于阿昔洛韦眼部给药:配方和角膜及巩膜通透性。

Soluplus micelles for acyclovir ocular delivery: Formulation and cornea and sclera permeability.

机构信息

Departamento de Farmacología, Farmacia y Tecnología Farmacéutica, R+D Pharma Group (GI-1645), Facultad de Farmacia and Health Research Institute of Santiago de Compostela (IDIS), Universidade de Santiago de Compostela, 15782 Santiago de Compostela, Spain.

Departamento de Farmacología, Farmacia y Tecnología Farmacéutica, R+D Pharma Group (GI-1645), Facultad de Farmacia and Health Research Institute of Santiago de Compostela (IDIS), Universidade de Santiago de Compostela, 15782 Santiago de Compostela, Spain.

出版信息

Int J Pharm. 2018 Dec 1;552(1-2):39-47. doi: 10.1016/j.ijpharm.2018.09.053. Epub 2018 Sep 22.

Abstract

Nearly 20% of people affected by the herpes simplex virus (HSV) suffer from vision problems. The virus can infect all layers of the cornea or cause inflammatory diseases of the sclera. The aim of this work was to test whether encapsulation of acyclovir in Soluplus or Solutol polymeric micelles increases its solubility, corneal permeability and sclera penetration. The aqueous solubility of acyclovir is known to be low, and therefore approaches that increase both its solubility and ability to penetrate through the eye may favor the efficacy of the treatments. Copolymer dispersions (covering wide range of concentrations) were prepared in water and PBS 7.4 and characterized regarding size and Z-potential (close to zero). Solutol micelles increased their size when the drug was incorporated (135 vs. 19 nm), while Soluplus micelles showed little difference (137 nm). Only Soluplus micelles significantly enhanced acyclovir solubility and withstood dilution stability tests. Soluplus (12-20%) formulations showed a progressive increase in viscoelasticity as temperature rose, which may allow for easy dropping onto the eye and subsequent retention in the gel form. Drug permeability through bovine cornea and sclera was investigated in detail. Although similar permeability coefficients were recorded for the drug when applied as the free drug in solution or formulated in Soluplus micelles, the micelle formulation significantly shortened the permeation lag time through the cornea. Moreover, Soluplus micelles were advantageous compared to the drug solution in terms of greater amount of acyclovir accumulated in both cornea and sclera, and higher steady state flux. If compared with cornea, the amounts of drug permeated through the sclera were approx. 10 times greater, which opens the possibility of drug delivery to the posterior eye segment.

摘要

近 20%的单纯疱疹病毒 (HSV) 感染者会出现视力问题。该病毒可感染角膜的所有层或引起巩膜的炎症性疾病。本工作旨在测试阿昔洛韦包封在 Soluplus 或 Solutol 聚合物胶束中是否能提高其溶解度、角膜通透性和巩膜穿透性。阿昔洛韦的水溶性已知较低,因此,增加其溶解度和穿透眼部能力的方法可能有利于治疗效果。共聚物分散体(涵盖广泛浓度范围)在水中和 PBS 7.4 中制备,并对其粒径和 Zeta 电位(接近零)进行了表征。当药物被包封时,Soluol 胶束的粒径增加(135 对 19nm),而 Soluplus 胶束的粒径变化不大(137nm)。只有 Soluplus 胶束能显著提高阿昔洛韦的溶解度,并能耐受稀释稳定性测试。Soluplus(12-20%)制剂的粘性随温度升高呈渐进性增加,这可能使其易于滴入眼部并在凝胶形式下保持滞留。详细研究了药物透过牛角膜和巩膜的渗透性。尽管以游离药物溶液或 Soluplus 胶束制剂形式应用时,药物的渗透系数相似,但胶束制剂显著缩短了药物透过角膜的渗透滞后时间。此外,与药物溶液相比,Soluplus 胶束在角膜和巩膜中累积的阿昔洛韦量更大,稳态通量更高,具有优势。与角膜相比,药物透过巩膜的量约增加 10 倍,这为药物递送至后眼部段开辟了可能性。

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