血脑屏障靶向脂质纳米粒子改善了铁前列素-1对实验性中风模型脑缺血损伤的神经保护作用。

IF 4.6 2区 医学 Q1 NEUROSCIENCES
Wenjuan Shi , Shuhua Yuan , Guohua Cheng , Huiling Zhang , Ke Jian Liu , Xunming Ji , Libo Du , Zhifeng Qi
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引用次数: 0

摘要

脑缺血中风是一种死亡率和致残率都很高的严重疾病。然而,临床上用于缺血性脑卒中的神经保护药物却寥寥无几。造成这种失败的原因主要有两个:难以穿透血脑屏障(BBB)和在血液循环中容易失活。铁氧化是一种与脂质氧化相关的细胞死亡,在脑缺血再灌注损伤中发挥着重要作用。我们利用从狂犬病毒糖蛋白中提取的多肽 RVG29 制备了 BBB 靶向脂质纳米颗粒(T-LNPs),以研究 T-LNPs 是否能改善铁锈素-1(Fer1,一种铁氧化抑制剂)对脑缺血损伤的神经保护作用。在体外 BBB 模型中,T-LNPs 在缺氧/葡萄糖暴露后能明显增加 BBB 穿透力;在脑缺血鼠模型中,T-LNPs 在给药后 6 小时能增强荧光在脑组织中的分布。此外,T-LNPs 封装 Fer1(T-LNPs-Fer1)通过维持脑缺血后神经元细胞中 NADPH 氧化酶 4(NOX4)和谷胱甘肽过氧化物酶 4(GPX4)信号的平衡,显著增强了 Fer1 对铁嗜酸性中毒的抑制作用。与未封装的单独 Fer1 相比,T-LNPs-Fer1 能显著抑制神经元中的氧化应激[血红素加氧酶-1 的表达和丙二醛(脂质 ROS 反应的产物)],并缓解缺血诱导的神经元细胞死亡。此外,与 Fer1 处理的脑缺血小鼠相比,T-LNPs-Fer1 在 45 分钟缺血/24 小时再灌注后可明显减轻脑梗塞并改善行为功能。这些研究结果表明,T-LNPs有助于Fer1穿透BBB,提高了Fer1对实验性脑卒中脑缺血损伤的神经保护作用,为开发治疗缺血性脑卒中的临床药物提供了可行的转化策略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Blood brain barrier-targeted lipid nanoparticles improved the neuroprotection of Ferrostatin-1 against cerebral ischemic damage in an experimental stroke model

Blood brain barrier-targeted lipid nanoparticles improved the neuroprotection of Ferrostatin-1 against cerebral ischemic damage in an experimental stroke model

Cerebral ischemic stroke is a serious disease with high mortality and disability rates. However, few neuroprotective drugs have been used for ischemic stroke in the clinic. Two main reasons may be responsible for this failure: difficulty in penetrating the blood-brain barrier (BBB) and easily inactivated in the blood circulation. Ferroptosis, a lipid oxidation-related cell death, plays significant roles in cerebral ischemia-reperfusion injury. We utilized RVG29, a peptide derived from Rabies virus glycoprotein, to obtain BBB-targeted lipid nanoparticles (T-LNPs) in order to investigate whether T-LNPs improved the neuroprotective effects of Ferrostatin-1 (Fer1, an inhibitor of ferroptosis) against cerebral ischemic damage. T-LNPs significantly increased BBB penetration following oxygen/glucose deprivation exposure in an in vitro BBB model and enhanced the fluorescence distribution in brain tissues at 6 h post-administration in a cerebral ischemic murine model. Moreover, T-LNPs encapsulated Fer1 (T-LNPs-Fer1) significantly enhanced the inhibitory effects of Fer1 on ferroptosis by maintaining the homeostasis of NADPH oxidase 4 (NOX4) and glutathione peroxidase 4 (GPX4) signals in neuronal cells after cerebral ischemia. T-LNPs-Fer1 significantly suppressed oxidative stress [heme oxygenase-1 expression and malondialdehyde (the product of lipid ROS reaction)] in neurons and alleviated ischemia-induced neuronal cell death, compared to Fer1 alone without encapsulation. Furthermore, T-LNPs-Fer1 significantly reduced cerebral infarction and improved behavior functions compared to Fer1-treated cerebral ischemic mice after 45-min ischemia/24-h reperfusion. These findings showed that the T-LNPs helped Fer1 penetrate the BBB and improved the neuroprotection of Fer1 against cerebral ischemic damage in experimental stroke, providing a feasible translational strategy for the development of clinical drugs for the treatment of ischemic stroke.

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来源期刊
Experimental Neurology
Experimental Neurology 医学-神经科学
CiteScore
10.10
自引率
3.80%
发文量
258
审稿时长
42 days
期刊介绍: Experimental Neurology, a Journal of Neuroscience Research, publishes original research in neuroscience with a particular emphasis on novel findings in neural development, regeneration, plasticity and transplantation. The journal has focused on research concerning basic mechanisms underlying neurological disorders.
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