Combat Wound Repair Division, United States Army Institute of Surgical Research, JBSA Fort Sam Houston, Texas, 78234, San Antonio, USA.
AAPS PharmSciTech. 2020 Oct 2;21(7):265. doi: 10.1208/s12249-020-01798-7.
This study used dual asymmetric centrifugation (DAC) to produce a topical vehicle for Pirfenidone (Pf; 5-methyl-1-phenyl-2[1H]-pyridone)-a Food and Drug Administration-approved antifibrotic drug indicated for idiopathic fibrosis treatment. Pf was loaded (8 wt%) in a poloxamer nanoemulsion gel (PNG) formulation consisting of water (47.8 wt%), triacetin (27.6 wt%), poloxamer 407 (P407, 13.8 wt%), polysorbate 80 (1.8 wt%), and benzyl alcohol (0.9 wt%). To our knowledge, poloxamer gels are typically processed with either high-shear methods or temperature regulation and have not been emulsified using DAC. Using a single-step emulsification process, 2 min mixed at 2500 RPM resulted in the lowest Pf loading variability with a relative standard deviation (RSD) of 0.96% for a 1.5 g batch size. Batch sizes of 15 g and 100 g yield higher RSD of 4.18% and 3.05%, respectively, but still in compliance with USP guidelines. Ex vivo permeation in full thickness porcine skin after 24 h showed total Pf permeation of 404.90 ± 67.07 μg/cm. Tested in vitro on human dermal fibroblasts stimulated with transforming growth factor-beta 1 (TGF-β1), Pf-PNG resulted in a > 2 fold decrease in α-SMA expression over vehicle control demonstrating that formulated Pf retained its biological activity. One-month stability testing at 25°C/60% relative humidity (RH) and 40°C/75% RH showed that % drug content, release kinetics, and biological activity were largely unchanged for both conditions; however, pH decreased from 6.7 to 5.5 (25°C/60% RH) and 4.5 (40°C/75% RH) after 1 month. Overall, these data demonstrate the utility of DAC to rapidly and reproducibly prepare lab-scale batches of emulsified gels for pharmaceutical formulation development.
本研究采用双不对称离心(DAC)法制备了一种吡非尼酮(Pf;5-甲基-1-苯基-2[1H]-吡啶酮)的局部载体,Pf 是一种已获得美国食品和药物管理局批准的抗纤维化药物,用于特发性纤维化的治疗。Pf 以 8wt%的浓度负载于泊洛沙姆纳米乳凝胶(PNG)制剂中,该制剂包含水(47.8wt%)、三醋酸甘油酯(27.6wt%)、泊洛沙姆 407(P407,13.8wt%)、聚山梨酯 80(1.8wt%)和苯甲醇(0.9wt%)。据我们所知,通常使用高剪切方法或温度调节来处理泊洛沙姆凝胶,而没有使用 DAC 对其进行乳化。通过一步乳化工艺,在 2500 RPM 下混合 2 分钟,可获得最低的 Pf 负载变异性,对于 1.5 g 批次大小,相对标准偏差(RSD)为 0.96%。对于 15 g 和 100 g 的批次大小,RSD 分别为 4.18%和 3.05%,但仍符合 USP 指南。在 24 小时后,在全厚猪皮上进行的体外渗透实验显示,Pf 的总渗透量为 404.90±67.07μg/cm。在体外用人真皮成纤维细胞进行转化生长因子-β1(TGF-β1)刺激试验,Pf-PNG 使 α-SMA 表达减少了 2 倍以上,与载体对照相比,表明所形成的 Pf 保留了其生物活性。在 25°C/60%相对湿度(RH)和 40°C/75%RH 下进行一个月的稳定性测试表明,在这两种条件下,药物含量、释放动力学和生物活性的百分比基本保持不变;然而,在 1 个月后,pH 值从 6.7 分别降至 5.5(25°C/60%RH)和 4.5(40°C/75%RH)。总体而言,这些数据表明 DAC 可快速且重现性地制备用于药物制剂开发的实验室规模的乳化凝胶批次。
