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利用铒:钇铝石榴石(Er:YAG)分激光消融实现靶向性的皮肤依那西普递送。

Targeted cutaneous delivery of etanercept using Er:YAG fractional laser ablation.

机构信息

School of Pharmaceutical Sciences, University of Geneva, CMU - 1 Rue Michel Servet 1211, Geneva, Switzerland.

Pantec Biosolutions AG, Industriering 21, 9491 Ruggell, Liechtenstein.

出版信息

Int J Pharm. 2020 Apr 30;580:119234. doi: 10.1016/j.ijpharm.2020.119234. Epub 2020 Mar 16.

Abstract

The aim was to investigate the feasibility of using Er:YAG fractional laser ablation to enable topical cutaneous delivery of etanercept (ETA). Preliminary investigations into the effect of fluence on micropore depth, measured by full-field optical coherence tomography, were followed by quantitative experiments to determine ETA delivery and its cutaneous biodistribution from solution and hydrogel formulations. Visualization studies were performed using confocal laser scanning microscopy and an ETA-fluorescein conjugate. Micropore depth was linearly dependent on laser fluence. However, use of a single pulse or "pulse stacking" (i.e. multiple pulses) to apply a given fluence affected pore depth; this was accommodated mathematically by including a "stacking factor". ETA delivery into porated skin from solution and 0.8% Carbopol® formulations was equivalent: increasing ETA content in the gels from 0.5 to 1 and 2% increased ETA delivery linearly (Formulations 7-9: 5.12 ± 0.95 to 7.48 ± 1.45 and 11.2 ± 2.2 µg/cm, respectively; 10% FAA, 89.9 J/cm, 5 ppp); occlusion further increased ETA delivery from Formulation 9 to 23.17 ± 6.62 µg/cm. Cutaneous biodistribution studies demonstrated that ETA was delivered in therapeutically relevant amounts to the epidermis and dermis. Topical laser-assisted delivery of ETA might expand its range of clinical indications to include recalcitrant but not widespread psoriatic plaques (clinical trial underway).

摘要

目的是研究使用 Er:YAG 分束激光消融来实现依那西普 (ETA) 的局部皮肤递药的可行性。初步研究了激光能量密度对全光纤相干断层扫描测量的微孔深度的影响,然后进行了定量实验,以确定从溶液和水凝胶制剂中输送 ETA 及其在皮肤中的生物分布。使用共聚焦激光扫描显微镜和 ETA-荧光素缀合物进行可视化研究。微孔深度与激光能量密度呈线性相关。然而,使用单个脉冲或“脉冲堆积”(即多个脉冲)施加给定的能量密度会影响孔深度;这通过包括“堆积因子”在数学上得到了适应。从溶液和 0.8% Carbopol®制剂到穿孔皮肤的 ETA 输送是等效的:将凝胶中 ETA 的含量从 0.5%增加到 1%和 2%,使 ETA 的输送量呈线性增加(制剂 7-9:5.12±0.95 至 7.48±1.45 和 11.2±2.2µg/cm,分别为 10% FAA,89.9J/cm,5 个脉冲);闭塞进一步增加了制剂 9 至 23.17±6.62µg/cm 的 ETA 输送。皮肤生物分布研究表明,ETA 以治疗相关的量递送至表皮和真皮。局部激光辅助输送 ETA 可能会扩大其临床应用范围,包括顽固但不广泛的银屑病斑块(正在进行临床试验)。

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