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创伤性脑损伤后通过血管闭塞实现基于脂质纳米颗粒的药物载体经血脑屏障的尺寸选择性转运

Size-Selective Transfer of Lipid Nanoparticle-Based Drug Carriers Across the Blood Brain Barrier Via Vascular Occlusions Following Traumatic Brain Injury.

作者信息

Khalin Igor, Adarsh Nagappanpillai, Schifferer Martina, Wehn Antonia, Groschup Bernhard, Misgeld Thomas, Klymchenko Andrey, Plesnila Nikolaus

机构信息

Institute for Stroke and Dementia Research, University of Munich Medical Center, 81377, Munich, Germany.

Cluster for Systems Neurology, Munich, Germany.

出版信息

Small. 2022 May;18(18):e2200302. doi: 10.1002/smll.202200302. Epub 2022 Apr 5.

Abstract

The current lack of understanding about how nanocarriers cross the blood-brain barrier (BBB) in the healthy and injured brain is hindering the clinical translation of nanoscale brain-targeted drug-delivery systems. Here, the bio-distribution of lipid nano-emulsion droplets (LNDs) of two sizes (30 and 80 nm) in the mouse brain after traumatic brain injury (TBI) is investigated. The highly fluorescent LNDs are prepared by loading them with octadecyl rhodamine B and a bulky hydrophobic counter-ion, tetraphenylborate. Using in vivo two-photon and confocal imaging, the circulation kinetics and bio-distribution of LNDs in the healthy and injured mouse brain are studied. It is found that after TBI, LNDs of both sizes accumulate at vascular occlusions, where specifically 30 nm LNDs extravasate into the brain parenchyma and reach neurons. The vascular occlusions are not associated with bleedings, but instead are surrounded by processes of activated microglia, suggesting a specific opening of the BBB. Finally, correlative light-electron microscopy reveals 30 nm LNDs in endothelial vesicles, while 80 nm particles remain in the vessel lumen, indicating size-selective vesicular transport across the BBB via vascular occlusions. The data suggest that microvascular occlusions serve as "gates" for the transport of nanocarriers across the BBB.

摘要

目前,对于纳米载体如何在健康和受损大脑中穿过血脑屏障(BBB)缺乏了解,这阻碍了纳米级脑靶向给药系统的临床转化。在此,研究了两种尺寸(30和80纳米)的脂质纳米乳滴(LNDs)在小鼠创伤性脑损伤(TBI)后脑内的生物分布。通过用十八烷基罗丹明B和一种庞大的疏水性抗衡离子四苯基硼酸盐加载LNDs来制备高荧光LNDs。利用体内双光子和共聚焦成像,研究了LNDs在健康和受损小鼠脑内的循环动力学和生物分布。研究发现,TBI后,两种尺寸的LNDs都在血管闭塞处积聚,其中30纳米的LNDs特别地渗入脑实质并到达神经元。这些血管闭塞与出血无关,而是被活化的小胶质细胞的突起包围,这表明血脑屏障有特定的开放。最后,相关光电子显微镜显示30纳米的LNDs在内皮小泡中,而80纳米的颗粒留在血管腔内,表明通过血管闭塞存在跨血脑屏障的尺寸选择性小泡运输。数据表明,微血管闭塞充当纳米载体跨血脑屏障运输的“大门”。

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