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开发并表征了一种干储库-水凝胶形成型微针复合材料,用于头孢唑林的微创给药。

Development and characterization of a dry reservoir-hydrogel-forming microneedles composite for minimally invasive delivery of cefazolin.

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. 2022 Apr 5;617:121593. doi: 10.1016/j.ijpharm.2022.121593. Epub 2022 Feb 16.

Abstract

Cefazolin (CFZ) is one of the most extensively used cephalosporins. This antibiotic exerts its bactericidal activity by interfering with bacterial cell wall formation, leading to bacteriolysis. CFZ is highly polar, resulting in the drug having poor oral bioavailability. Accordingly, the antibiotic is administered via intramuscular or intravenous injections, which are both painful and invasive. Due to these limitations, there is an impetus to explore alternative drug delivery platforms which offer a minimally invasive approach to delivery CFZ into and across the skin. The current work presents the development of a composite pharmaceutical system composed of hydrogel-forming microneedles (MNs) in tandem with CFZ dry reservoirs. The hydrogel system was fabricated from Gantrez® S-97 and Carbopol® 974P NF crosslinked with PEG 10,000. Swelling kinetic studies showed that the hydrogel system developed was capable of achieving 4000% swelling in PBS pH 7.4. In addition, results from a solute diffusion study showed that CFZ was able to achieve ≈100% cumulative permeation across the swollen hydrogel film. When formulated into MNs, the hydrogel system was capable of breaching the stratum corneum, resulting in intradermal insertion of the hydrogel forming MNs into ex vivo neonatal porcine skin, as evidenced from optical coherence tomography. In addition, two different CFZ loaded dry reservoirs consisting of directly compressed tablets (DCT) and lyophilised (LYO) wafers were formulated and characterised. These dry reservoir systems showed fast dissolution, dissolving in phosphate buffer saline pH 7.4 in less than one minute. In vitro permeation studies, using full thickness ex vivo neonatal porcine skin were conducted. HPLC analysis demonstrated the dry reservoir combination consisting of DCT with hydrogel-forming MNs was capable of achieving up to 80 µg CFZ delivery into the epidermis within 2 h of application. In addition, DCT reservoir coupled with hydrogel-forming MNs were able to deliver CFZ up to 1.8 mg into and across the skin at 24 h. Should this system be translated into clinical practice, it may provide a minimally invasive strategy to administer CFZ for the treatment of infections such as septic arthritis, osteomyelitis and cellulitis.

摘要

头孢唑林(CFZ)是应用最广泛的头孢菌素之一。这种抗生素通过干扰细菌细胞壁的形成发挥杀菌作用,导致细菌溶解。CFZ 具有很强的极性,导致药物的口服生物利用度很差。因此,该抗生素通过肌内或静脉注射给药,这两种方式既痛苦又具有侵入性。由于这些限制,人们有动力探索替代药物输送平台,为将 CFZ 递送到皮肤中并穿过皮肤提供微创方法。目前的工作提出了一种由水凝胶形成的微针(MN)与 CFZ 干粉库串联组成的复合药物系统的开发。水凝胶系统由 Gantrez® S-97 和 Carbopol® 974P NF 与 PEG 10,000 交联制成。溶胀动力学研究表明,所开发的水凝胶系统能够在 PBS pH 7.4 中达到 4000%的溶胀。此外,溶质扩散研究的结果表明,CFZ 能够实现 ≈100%的累积渗透穿过溶胀的水凝胶膜。当制成 MN 时,水凝胶系统能够穿透角质层,导致水凝胶形成的 MN 插入离体新生猪皮的真皮中,这可以从光学相干断层扫描中得到证明。此外,还制备和表征了两种不同的 CFZ 负载干粉库,包括直接压片(DCT)和冻干(LYO)片。这些干粉库系统显示出快速溶解的特点,在不到一分钟的时间内在磷酸盐缓冲盐水 pH 7.4 中溶解。使用全厚度离体新生猪皮进行了体外渗透研究。HPLC 分析表明,由 DCT 与水凝胶形成的 MN 组成的干粉库组合能够在 2 小时的应用内将高达 80µg CFZ 递送到表皮中。此外,DCT 储库与水凝胶形成的 MN 联合能够在 24 小时内将 CFZ 递送到皮肤内部和外部,达到 1.8mg。如果将该系统转化为临床实践,它可能为治疗感染(如脓毒性关节炎、骨髓炎和蜂窝织炎)提供一种微创的 CFZ 给药策略。

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