在黑质上聚焦超声波可安全地通过鼻内和血液循环向多巴胺能神经元递送神经肽多聚物纳米颗粒介导的基因。

0 MATERIALS SCIENCE, MULTIDISCIPLINARY

Discover nano Pub Date : 2024-04-02 DOI:10.1186/s11671-024-04005-9

Juan U Mascotte-Cruz, Arturo Vera, Lorenzo Leija, Francisco E Lopez-Salas, Michael Gradzielski, Joachim Koetz, Bismark Gatica-García, C P Rodríguez-Oviedo, Irais E Valenzuela-Arzeta, Lourdes Escobedo, David Reyes-Corona, M E Gutierrez-Castillo, Minerva Maldonado-Berny, Armando J Espadas-Alvarez, Carlos E Orozco-Barrios, Daniel Martinez-Fong

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引用次数: 0

摘要

在帕金森病的临床前试验中，脑内注射神经紧张素-多聚物纳米粒子可有效转染黑质多巴胺能神经元，因为它们不能穿过血脑屏障（BBB）。因此，本研究旨在用聚焦超声（FUS）打开黑质的血脑屏障，实现全身和鼻内转染，并评估其对大鼠的有害影响。全身注射伊文思蓝的结果显示，双脉冲 FUS 打开了黑质 BBB。因此，在 FUS 30 分钟后，经颈内动脉、眶后静脉窦或鼻粘膜输送 35 μL 含有绿色荧光蛋白质粒（平均大小为 79.6 nm，Zeta 电位为 + 1.3 mV）的神经肽多聚物纳米颗粒，可在黑质的酪氨酸羟化酶（+）细胞（多巴胺能神经元）中表达绿色荧光蛋白质粒。颈内动脉给药的转基因表达量最高，其次是鼻内给药和静脉给药。然而，FUS会引起神经炎症，表现为淋巴细胞浸润（分化簇45呈阳性）、小胶质细胞活化（电离钙结合适配分子1呈阳性）、神经毒性A1星形胶质细胞（胶质纤维酸性蛋白和补体成分3呈阳性）和神经营养性A2星形胶质细胞（胶质纤维酸性蛋白和S100钙结合蛋白A10呈阳性），FUS作用15天后结束。多巴胺能神经元和轴突突起减少，但在转染后第15天恢复了基础值，这与运动行为的减少和恢复相关。总之，FUS 会引起短暂的神经炎症和可逆的神经元损伤，但可以通过全身和鼻内转染两种黑质的多巴胺能神经元。因此，FUS 可以推动神经肽-多聚物纳米技术进入帕金森病的临床试验阶段。

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Focused ultrasound on the substantia nigra enables safe neurotensin-polyplex nanoparticle-mediated gene delivery to dopaminergic neurons intranasally and by blood circulation.

Neurotensin-polyplex nanoparticles provide efficient gene transfection of nigral dopaminergic neurons when intracerebrally injected in preclinical trials of Parkinson's disease because they do not cross the blood-brain barrier (BBB). Therefore, this study aimed to open BBB with focused ultrasound (FUS) on the substantia nigra to attain systemic and intranasal transfections and evaluate its detrimental effect in rats. Systemically injected Evans Blue showed that a two-pulse FUS opened the nigral BBB. Accordingly, 35 μL of neurotensin-polyplex nanoparticles encompassing the green fluorescent protein plasmid (79.6 nm mean size and + 1.3 mV Zeta-potential) caused its expression in tyrosine hydroxylase(+) cells (dopaminergic neurons) of both substantiae nigrae upon delivery via internal carotid artery, retro-orbital venous sinus, or nasal mucosa 30 min after FUS. The intracarotid delivery yielded the highest transgene expression, followed by intranasal and venous administration. However, FUS caused neuroinflammation displayed by infiltrated lymphocytes (positive to cluster of differentiation 45), activated microglia (positive to ionized calcium-binding adaptor molecule 1), neurotoxic A1 astrocytes (positive to glial fibrillary acidic protein and complement component 3), and neurotrophic A2 astrocytes (positive to glial fibrillary acidic protein and S100 calcium-binding protein A10), that ended 15 days after FUS. Dopaminergic neurons and axonal projections decreased but recuperated basal values on day 15 after transfection, correlating with a decrease and recovery of locomotor behavior. In conclusion, FUS caused transient neuroinflammation and reversible neuronal affection but allowed systemic and intranasal transfection of dopaminergic neurons in both substantiae nigrae. Therefore, FUS could advance neurotensin-polyplex nanotechnology to clinical trials for Parkinson's disease.

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Discover nano

CiteScore

0.70

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0.00%

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