Novel long-acting treatment for schizophrenia based on paliperidone dissolving and implantable microarray patches

IF 4.4 2区医学 Q1 PHARMACOLOGY & PHARMACY European Journal of Pharmaceutics and Biopharmaceutics Pub Date : 2024-09-08 DOI:10.1016/j.ejpb.2024.114481

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Abstract

Schizophrenia is a severe mental disorder that affects millions of people worldwide. Several atypical antipsychotic medications, including paliperidone (PPD), has been developed and proven effective in treating it. To date, four PPD extended-release products have been launched commercially, providing up to six months of therapeutic effect with a single administration. However, the need for hospital injections by professional healthcare workers not only lead to poor patients’ adherence, but also put additional pressure on the healthcare system. Therefore, three PPD microarray patch (PPD MAP) systems based on dissolving microneedle technology and implantable microneedle technology were developed in this work. The two dissolving microarray patch systems contained either PPD crude drug (PPD DMAP-CD) or PPD nanocrystal (PPD DMAP-NC) and the implantable MAP contained PPD crude drug (PPD IMAP). All three types of PPD MAPs showed excellent mechanical and insertion properties as they achieved over 256 µm insertion depth in skin model. In vitro release study showed that PPD released from IMAP in a much more sustained manner (up to 14 days) than PPD did from DMAPs (7 days), with only 20 % initial burst release from IMAP compared with 43–71 % from DMAPs. The MAP dissolution study showed that both DMAPs can be immediately dissolved within less than 3 min once inserted into the skin, indicating a faster action potential compared with IMAP. Ex vivo delivery study showed that 1.68 ± 0.23 mg, 1.39 ± 0.07 mg, and 1.18 ± 0.12 mg were delivered from DMAP-CD, DMAP-NC and IMAP, respectively, demonstrating that over 50 % and up to 70 % of PPD in the MAPs can be delivered into the skin. The IMAP offers most sustained release of PPD whereas DMAP-NC exhibits fastest PPD release (11.19 % vs 20.01 % into Franz cell receiver compartment over 24 h). This work presents a promising alternative for the sustained delivery of antipsychotic drugs, allowing for patient self-administration and extended release concurrently. Patients may potentially use both DMAP and IMAP to achieve a sustained release of PPD while also avoid having an initial therapeutic lag.

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基于帕潘立酮溶解和植入式微阵列贴片的新型精神分裂症长效疗法

精神分裂症是一种严重的精神障碍，影响着全球数百万人。包括帕利哌酮（PPD）在内的几种非典型抗精神病药物已被开发出来，并被证明对治疗该病有效。迄今为止，已有四种帕利哌酮缓释产品投入市场，一次给药可提供长达六个月的疗效。然而，专业医护人员需要到医院注射，这不仅导致患者依从性差，也给医疗系统带来额外压力。因此，本研究开发了三种基于溶解微针技术和植入微针技术的 PPD 微阵列贴片（PPD MAP）系统。两种溶解型微阵列贴片系统含有 PPD 原药（PPD DMAP-CD）或 PPD 纳米晶体（PPD DMAP-NC），而植入型 MAP 则含有 PPD 原药（PPD IMAP）。这三种 PPD MAP 在皮肤模型中的插入深度均超过 256 微米，显示出优异的机械和插入性能。体外释放研究表明，PPD 从 IMAP 中释放的时间（长达 14 天）比从 DMAP 中释放的时间（7 天）要长得多，IMAP 的初始迸发释放率仅为 20%，而 DMAP 为 43-71%。MAP 溶解研究表明，两种 DMAP 进入皮肤后都能在 3 分钟内立即溶解，这表明与 IMAP 相比，DMAP 的动作电位更快。体内释放研究显示，DMAP-CD、DMAP-NC 和 IMAP 分别释放了 1.68 ± 0.23 毫克、1.39 ± 0.07 毫克和 1.18 ± 0.12 毫克的 PPD，表明 MAP 中超过 50% 和高达 70% 的 PPD 可以释放到皮肤中。IMAP 可提供最持久的 PPD 释放，而 DMAP-NC 则表现出最快的 PPD 释放速度（在 24 小时内进入 Franz 细胞接收区的 PPD 释放率为 11.19% 对 20.01%）。这项研究为抗精神病药物的持续给药提供了一种很有前景的替代方法，病人可以同时自行给药和延长释放时间。患者有可能同时使用 DMAP 和 IMAP 来实现 PPD 的持续释放，同时还能避免最初的治疗滞后。

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来源期刊

European Journal of Pharmaceutics and Biopharmaceutics 医学-药学

CiteScore

8.80

自引率

4.10%

发文量

211

审稿时长

36 days

期刊介绍： The European Journal of Pharmaceutics and Biopharmaceutics provides a medium for the publication of novel, innovative and hypothesis-driven research from the areas of Pharmaceutics and Biopharmaceutics. Topics covered include for example: Design and development of drug delivery systems for pharmaceuticals and biopharmaceuticals (small molecules, proteins, nucleic acids) Aspects of manufacturing process design Biomedical aspects of drug product design Strategies and formulations for controlled drug transport across biological barriers Physicochemical aspects of drug product development Novel excipients for drug product design Drug delivery and controlled release systems for systemic and local applications Nanomaterials for therapeutic and diagnostic purposes Advanced therapy medicinal products Medical devices supporting a distinct pharmacological effect.