Huang Hao, Xuan Yan, Ma Zeng-Chun
GCP Institutional Office, The First People's Hospital of Neijiang, Neijiang, Sichuan, 641000, People's Republic of China.
Department of Clinical Pharmacy, Chengdu Qingbaijiang District People's Hospital, Chengdu, Sichuan, 610399, People's Republic of China.
Nanotechnol Sci Appl. 2025 Jul 28;18:319-358. doi: 10.2147/NSA.S500407. eCollection 2025.
Ferulic acid (FA) exhibits therapeutic potential for various disorders, but its clinical application is hindered by poor bioavailability and solubility. This study aimed to develop and evaluate FA-loaded lipid nanoparticles (FA-LNPs) as a safe and efficient drug delivery system.
FA-LNPs were prepared via an optimized active loading method. The Morris water maze test was conducted to evaluate FA efficacy against LPS-induced cognitive impairment in rats. Comprehensive neurotoxicity assessment was performed in three brain regions (striatum, hippocampus, and cerebellum-brain stem) using multiple staining techniques (LFB, GFAP, IBA-1, and Fluoro-Jade) to evaluate myelin integrity, glial activation, and neuronal degeneration. Acute toxicity, pharmacokinetics, and network pharmacology analysis were conducted to assess safety profiles and potential mechanisms.
FA-LNPs were successfully prepared using an optimized active loading method, achieving high drug loading (≥4 mg/mL), superior encapsulation efficiency (EE%) ≥80%, and uniform particle size distribution (<200 nm, PDI=0.053), zeta potential of +5.97 mV (Quality Factor = 1.701), excellent storage stability over two weeks, and was scaled up for batch production. The Morris water maze test revealed an effective FA concentration of 50 mg/kg, with FA-LNPs achieving 46.5 mg/kg through active loading method. Toxicological studies demonstrated favorable safety profiles. Pharmacokinetic analysis showed a prolonged elimination half-life (12.8 ± 1.88 hours) and moderate systemic clearance (0.535 ± 0.0851 L/h/kg). Short-term administration did not elicit significant neuroprotection. Network pharmacology analysis identified 141 potential therapeutic targets and five key proteins (EGFR, ESR1, PTGS2, CTNNB1, and STAT3), with molecular docking confirming favorable binding energies (-7.6 to -5.2 kcal/mol).
FA-LNPs enhanced FA's bioavailability without apparent systemic toxicity or neurotoxicity. While safe for short-term use, longer treatment durations may be necessary to observe potential neuroprotective benefits and toxicity. This study provides a foundation for further investigation of FA-LNPs as a promising drug delivery system for neurological disorders.
阿魏酸(FA)对多种疾病具有治疗潜力,但其临床应用受到生物利用度低和溶解度差的阻碍。本研究旨在开发和评估载有FA的脂质纳米颗粒(FA-LNPs)作为一种安全有效的药物递送系统。
通过优化的主动载药方法制备FA-LNPs。进行Morris水迷宫试验,以评估FA对脂多糖(LPS)诱导的大鼠认知障碍的疗效。使用多种染色技术(LFB、GFAP、IBA-1和Fluoro-Jade)在三个脑区(纹状体、海马体和小脑-脑干)进行全面的神经毒性评估,以评估髓鞘完整性、胶质细胞活化和神经元变性。进行急性毒性、药代动力学和网络药理学分析,以评估安全性概况和潜在机制。
采用优化的主动载药方法成功制备了FA-LNPs,实现了高载药量(≥4mg/mL)、优异的包封率(EE%)≥80%、粒径分布均匀(<200nm,PDI = 0.053)、zeta电位为+5.97mV(质量因子 = 1.701)、两周内具有优异的储存稳定性,并扩大规模进行批量生产。Morris水迷宫试验显示FA的有效浓度为50mg/kg,通过主动载药方法,FA-LNPs达到46.5mg/kg。毒理学研究表明其安全性良好。药代动力学分析显示消除半衰期延长(12.8±1.88小时),全身清除率适中(0.535±0.0851L/h/kg)。短期给药未引起明显的神经保护作用。网络药理学分析确定了141个潜在治疗靶点和5个关键蛋白(EGFR、ESR1、PTGS2、CTNNB1和STAT3),分子对接证实了良好的结合能(-7.6至-5.2kcal/mol)。
FA-LNPs提高了FA的生物利用度,且无明显的全身毒性或神经毒性。虽然短期使用安全,但可能需要更长的治疗时间来观察潜在的神经保护益处和毒性。本研究为进一步研究FA-LNPs作为一种有前途的神经系统疾病药物递送系统奠定了基础。
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