载姜黄素纳米结构脂质载体的研制及其对 Wistar 大鼠淀粉样β诱导阿尔茨海默病的作用。
Development of silibinin-loaded nanostructured lipid carriers for Alzheimer's disease induced by amyloid beta in Wistar rats.
机构信息
Department of Pharmaceutics, School of Pharmacy, Hamadan University of Medical Sciences, Hamadan, Iran.
Department of Physiology, School of Medicine, Hamadan University of Medical Sciences, Hamadan, Iran.
出版信息
J Mater Chem B. 2024 Nov 13;12(44):11426-11443. doi: 10.1039/d4tb00775a.
. The purpose of this study is to develop, optimize, and evaluate the effectiveness of orally administered silibinin-loaded nanostructured lipid carriers (SB-NLCs) in amyloid β-induced Alzheimer's disease in Wistar rats. . The emulsification-solvent evaporation method was used for preparing the NLCs, using stearic acid, triacetin, and Cremophor® RH40. The statistical optimization of SB-NLCs was done using the Box-Behnken design (BBD). Then, the following parameters were evaluated: zeta potential, average size, drug release, and drug entrapment efficiency. Physicochemical properties of the optimized SB-NLCs were determined by FTIR, DSC, and P-XRD. The behavioral (OFT, NOR, MWM), histological (H&E, Congo Red), and biochemical (TAC, MDA, GSH) tests were conducted on 48 male Wistar rats. . The findings showed that the mean particle size, zeta potential and entrapment efficiency of optimized SB-NLCs were 194.71 ± 14.06 nm, -12.46 ± 0.25 mV, and 72.13% ± 1.41, respectively. XRD and DSC studies confirmed a reduction in the crystallinity of SB which occurred due to its embedment in the nanostructured lipid. The FTIR results indicated the lack of existence of any chemical interaction between the carrier components and the drug. Drug release in the external environment was slow and steady. Drug-containing nanoparticles showed good stability during three months of storage at 4 °C. The behavioral test of OFT showed no significant change between groups. The group treated with SB-NLCs showed a markedly higher discrimination rate compared to the Aβ group ( < 0.001). The time of the SB-NLC treated group in the target area was considerably more than the time of the SB and Aβ groups, respectively ( < 0.01, < 0.001), in the MWM test. Histological and biochemical analysis revealed better results in the SB-NLC group as against the SB group. . SB-NLCs can be considered as a promising formulation for the proper treatment of Alzheimer's disease in the oral drug delivery system.
. 本研究旨在开发、优化并评估口服姜黄素负载纳米结构脂质载体(SB-NLCs)在 Wistar 大鼠淀粉样β诱导的阿尔茨海默病中的疗效。. 采用乳化-溶剂蒸发法制备 NLCs,使用硬脂酸、三乙酸甘油酯和 Cremophor® RH40。采用 Box-Behnken 设计(BBD)对 SB-NLCs 进行统计优化。然后,评估以下参数:zeta 电位、平均粒径、药物释放和药物包封效率。通过傅里叶变换红外光谱(FTIR)、差示扫描量热法(DSC)和粉末 X 射线衍射(P-XRD)对优化后的 SB-NLCs 的物理化学性质进行了测定。对 48 只雄性 Wistar 大鼠进行行为(OFT、NOR、MWM)、组织学(H&E、刚果红)和生化(TAC、MDA、GSH)检测。. 结果显示,优化后的 SB-NLCs 的平均粒径、zeta 电位和包封效率分别为 194.71±14.06nm、-12.46±0.25mV 和 72.13%±1.41。XRD 和 DSC 研究证实,SB 的结晶度降低,这是由于其嵌入纳米结构脂质所致。FTIR 结果表明载体成分与药物之间不存在任何化学相互作用。在外部环境中,药物释放缓慢且稳定。载药纳米粒子在 4°C 下储存三个月仍保持良好的稳定性。OFT 行为测试显示各组之间无显著差异。与 Aβ 组相比,SB-NLC 组的辨别率显著提高(<0.001)。MWM 测试中,SB-NLC 组在靶区的时间明显长于 SB 组和 Aβ 组(<0.01,<0.001)。组织学和生化分析显示,SB-NLC 组的结果优于 SB 组。. SB-NLCs 可被视为口服药物传递系统中治疗阿尔茨海默病的一种有前途的制剂。
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