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脂质纳米胶囊作为一种新型环鸟苷酸模拟物的药物传递系统的制剂开发和放大,用于视网膜药物传递。

Formulation development and upscaling of lipid nanocapsules as a drug delivery system for a novel cyclic GMP analogue intended for retinal drug delivery.

机构信息

RISE Research Institutes of Sweden, SE-151 36 Södertälje, Sweden; Faculty of Pharmaceutical Sciences, School of Health Sciences, University of Iceland, Hofsvallagata 53, IS-107 Reykjavík, Iceland.

RISE Research Institutes of Sweden, SE-151 36 Södertälje, Sweden.

出版信息

Int J Pharm. 2021 Jun 1;602:120640. doi: 10.1016/j.ijpharm.2021.120640. Epub 2021 Apr 24.

DOI:10.1016/j.ijpharm.2021.120640
PMID:33901599
Abstract

Lipid nanocapsules (LNCs) were prepared with a novel cyclic GMP analogue, DF003, intended for the treatment of neurodegenerative retinal degenerations. LNCs loaded with DF003 were prepared by a phase inversion method and characterized for particle size, polydispersity index, drug loading, entrapment efficiency, stability, and in vitro drug release. Particle size, PdI and zeta potential of selected optimized formulation were 76 ± 1.2 nm, 0.16 ± 0.02, and -11.6 ± 0.4 mV, respectively, with an entrapment efficiency of 69 ± 0.5%. The selected formulation showed a sustained drug release for up to 6 days in phosphate buffer as well as in vitreous components. Stability evaluation of LNCs in presence of vitreous components demonstrated structural stability and compatibility. Further, the nanoparticle preparation process was upscaled to 1000 times (10 L) of the typical lab scale (0.01 L). Product parameters were observed to be unaffected by the upscaling, demonstrating that the LNCs were of the same quality as those prepared at lab scale. Additionally, the manufacturing process was adapted and assessed for a continuous production of LNCs to leverage it for industrial viability. Overall, these findings reveal the remarkable potential of LNCs as drug delivery vehicles and their possibility for clinical translation.

摘要

脂质纳米胶囊 (LNCs) 是用一种新型的环鸟苷酸 analogue (DF003) 制备的,旨在治疗神经退行性视网膜变性。通过相转化法制备载有 DF003 的 LNCs,并对其粒径、多分散指数、药物载量、包封效率、稳定性和体外药物释放进行了表征。选择的优化配方的粒径、PdI 和 zeta 电位分别为 76±1.2nm、0.16±0.02 和-11.6±0.4mV,包封效率为 69±0.5%。该配方在磷酸盐缓冲液和玻璃体成分中表现出长达 6 天的持续药物释放。在玻璃体成分存在下对 LNCs 的稳定性评估表明其结构稳定且具有兼容性。此外,将纳米颗粒制备过程放大到典型实验室规模 (0.01 L) 的 1000 倍 (10 L)。观察到产品参数不受放大的影响,表明 LNCs 的质量与在实验室规模制备的相同。此外,还对 LNCs 的连续生产进行了适应性调整和评估,以实现其工业化可行性。总的来说,这些发现揭示了 LNCs 作为药物传递载体的巨大潜力及其在临床转化方面的可能性。

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