Luchi Li, Qonita Kurnia Anjani, Aaron R J Hutton, Mingshan Li, Akmal Hidayat Bin Sabri, Lalitkumar Vora, Yara A Naser, Yushi Tao, Helen O McCarthy, Ryan F Donnelly
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引用次数: 0
摘要
水凝胶形成的微针(MN)阵列是一种微创设备,可以穿透局部用药的主要障碍--角质层,而且不会造成疼痛。然而,与使用传统针头和注射器快速给药相比,使用水凝胶形成的微针阵列给药往往相对缓慢。因此,本研究首次将不同的物理和化学给药增强方法与基于 PVA 的水凝胶成型 MN 阵列相结合。使用布洛芬(IBU)钠作为模型药物,对所设计的系统的透皮给药程度进行了评估。研究了作为物理渗透增强技术的离子渗透(ITP)和热辅助给药技术。体内外研究表明,与单用 MN(约 1.63 毫克)相比,ITP(0.5 毫安/平方厘米)介导的组合策略在头 6 小时(约 5.11 毫克)和 6 小时(约 140.81 微克/毫升)分别显著增强了 IBU 钠的透皮渗透(p max)。这些策略不仅能迅速达到治疗水平(10-15 微克/毫升),还能使 IBU 钠持续释放至少 48 小时,从而有效减少给药次数,提高患者的依从性并减少 IBU 钠的副作用。
Evaluation of physical and chemical modifications to drug reservoirs for stimuli-responsive microneedles.
Hydrogel-forming microneedle (MN) arrays are minimally-invasive devices that can penetrate the stratum corneum, the main barrier to topical drug application, without causing pain. However, drug delivery using hydrogel-forming MN arrays tends to be relatively slow compared to rapid drug delivery using conventional needles and syringes. Therefore, in this work, for the first time, different physical and chemical delivery enhancement methods were employed in combination with PVA-based hydrogel-forming MN arrays. Using a model drug, ibuprofen (IBU) sodium, the designed systems were assessed in terms of the extent of transdermal delivery. Iontophoresis (ITP) and heat-assisted drug delivery technology were investigated as physical permeation enhancement techniques. Ex vivo studies demonstrated that the ITP (0.5 mA/cm2)-mediated combination strategy significantly enhanced the transdermal permeation of IBU sodium over the first 6 h (~ 5.11 mg) when compared to MN alone (~ 1.63 mg) (p < 0.05). In contrast, heat-assisted technology showed almost no promoting effect on transdermal delivery. Furthermore, IBU sodium-containing rapidly dissolving lyophilised and effervescent reservoirs, classified as chemical modification methods, were prepared. Both strategies achieved rapid and effective ex vivo IBU sodium permeation, equating to ~ 78% (30.66 mg) and ~ 71% (28.43 mg) from lyophilised and effervescent reservoirs, respectively. Moreover, in vivo pharmacokinetic studies showed that the IBU sodium plasma concentration within lyophilised and effervescent groups reached a maximum concentration (Cmax) at 4 h (~ 282.15 µg/mL) and 6 h (~ 140.81 µg/mL), respectively. These strategies not only provided rapid achievement of therapeutic levels (10-15 µg/ml), but also resulted in sustained release of IBU sodium for at least 48 h, which could effectively reduce the frequency of administration, thereby improving patient compliance and reducing side effects of IBU sodium.
期刊介绍:
The journal provides a unique forum for scientific publication of high-quality research that is exclusively focused on translational aspects of drug delivery. Rationally developed, effective delivery systems can potentially affect clinical outcome in different disease conditions.
Research focused on the following areas of translational drug delivery research will be considered for publication in the journal.
Designing and developing novel drug delivery systems, with a focus on their application to disease conditions;
Preclinical and clinical data related to drug delivery systems;
Drug distribution, pharmacokinetics, clearance, with drug delivery systems as compared to traditional dosing to demonstrate beneficial outcomes
Short-term and long-term biocompatibility of drug delivery systems, host response;
Biomaterials with growth factors for stem-cell differentiation in regenerative medicine and tissue engineering;
Image-guided drug therapy,
Nanomedicine;
Devices for drug delivery and drug/device combination products.
In addition to original full-length papers, communications, and reviews, the journal includes editorials, reports of future meetings, research highlights, and announcements pertaining to the activities of the Controlled Release Society.
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