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通过泡腾载粉空心微针和载纳米晶微针增强辛伐他汀的长效递送。

Enhanced long-acting simvastatin delivery via effervescent powder-carrying hollow microneedles and nanocrystal-loaded microneedles.

机构信息

School of Pharmacy, Queen's University Belfast, Medical Biology Centre, 97 Lisburn Road, Belfast BT9 7BL, UK.

School of Pharmacy, Queen's University Belfast, Medical Biology Centre, 97 Lisburn Road, Belfast BT9 7BL, UK.

出版信息

Int J Pharm. 2024 Nov 15;665:124691. doi: 10.1016/j.ijpharm.2024.124691. Epub 2024 Sep 14.

DOI:10.1016/j.ijpharm.2024.124691
PMID:39278288
Abstract

Hyperlipidemia and its associated cardiovascular complications are the major causes of mortality and disability worldwide. Simvastatin (SIM) is one of the most commonly prescribed lipid-lowering drugs for the treatment of hyperlipidemia by competitive inhibition of 3-hydroxy-3-methylglutaryl coenzyme A (HMG-CoA) reductase. However, the extensive first-pass metabolism leading to low oral bioavailability and frequent daily doses may lead to poor patient compliance and adverse effects caused by plasma fluctuations. To overcome these challenges, this work purposed two microneedle (MN) delivery strategies for the potential enhancement of SIM delivery. Firstly, nanocrystal (NC) formulations of SIM were investigated, followed by incorporation into a trilayer dissolving microneedle (DMN) design. Furthermore, a novel effervescent powder-carrying MN (EMN) design was developed to enhance intradermal delivery by incorporating the effervescent agents into the drug powder. Both MN approaches exhibited significantly improved permeation and in-skin deposition ability in the Franz cell study, with the ex vivo delivery efficiency of 64.33 ± 6.17 % and 40.11 ± 4.53 % for EMNs and DMNs, respectively. Most importantly, in vivo studies using a female Sprague-Dawley rat model confirmed the successful delivery of SIM from NCs-loaded DMNs (C = 287.39 ± 106.82 ng/mL) and EMNs (C = 203.05 ± 17.07 ng/mL) and maintain therapeutically relevant plasma concentrations for 15 days following a single application. The enhanced bioavailabilities of DMNs and EMNs were 24.28 % and 103.82 %, respectively, which were both significantly higher than that of conventional oral administration.

摘要

高脂血症及其相关心血管并发症是全球主要的死亡和残疾原因。辛伐他汀(SIM)是通过竞争性抑制 3-羟基-3-甲基戊二酰辅酶 A(HMG-CoA)还原酶来治疗高脂血症的最常用降脂药物之一。然而,广泛的首过代谢导致口服生物利用度低和需要频繁每日给药,可能导致患者顺应性差和血浆波动引起的不良反应。为了克服这些挑战,本工作提出了两种微针(MN)给药策略,以提高 SIM 的递送效果。首先,研究了 SIM 的纳米晶体(NC)制剂,然后将其纳入三层溶解微针(DMN)设计中。此外,开发了一种新型的泡腾粉载微针(EMN)设计,通过将泡腾剂纳入药物粉末中来增强皮内递送。在 Franz 细胞研究中,两种 MN 方法都表现出显著改善的渗透和皮内沉积能力,EMN 和 DMN 的体外递送效率分别为 64.33±6.17%和 40.11±4.53%。最重要的是,使用雌性 Sprague-Dawley 大鼠模型的体内研究证实了 NC 负载 DMN(C=287.39±106.82ng/mL)和 EMN(C=203.05±17.07ng/mL)从 SIM 成功递送,并在单次应用后 15 天内维持治疗相关的血浆浓度。DMN 和 EMN 的增强生物利用度分别为 24.28%和 103.82%,均显著高于常规口服给药。

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