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一种短暂性脑缺血发作的替代性光血栓形成模型。

An Alternative Photothrombotic Model of Transient Ischemic Attack.

作者信息

Kalyuzhnaya Y N, Logvinov A K, Pashkevich S G, Golubova N V, Seryogina E S, Potapova E V, Dremin V V, Dunaev A V, Demyanenko S V

机构信息

Laboratory of Molecular Neuroscience, Academy of Biology and Biotechnology, Southern Federal University, 194/1 Stachki Ave, Rostov-On-Don, 344090, Russia.

State Scientific Institution "Institute of Physiology, of the National Academy of Sciences of Belarus", Akademicheskaya Str., 28, 220072, Minsk, Belarus.

出版信息

Transl Stroke Res. 2024 Jul 29. doi: 10.1007/s12975-024-01285-2.

Abstract

Animal models mimicking human transient ischemic attack (TIA) and cerebral microinfarcts are essential tools for studying their pathogenetic mechanisms and finding methods of their treatment. Despite its advantages, the model of single arteriole photothrombosis requires complex experimental equipment and highly invasive surgery, which may affect the results of further studies. Hence, to achieve high translational potential, we focused on developing a TIA model based on photothrombosis of arterioles to combine good reproducibility and low invasiveness. For the first time, noninvasive laser speckle contrast imaging (LSCI) was used to monitor blood flow in cerebral arterioles and reperfusion was achieved. We demonstrate that irradiation of mouse cerebral cortical arterioles using a 532-nm laser with a 1-mm-wide beam at 2.4 or 3.7 mW for 55 or 40 s, respectively, after 15 mg/kg intravenous Rose Bengal administration, induces similar ischemia-reperfusion lesions resulting in microinfarct formation. The model can be used to study the pathogenesis of spontaneously developing cerebral microinfarcts in neurodegeneration. Reducing the exposure times by 10 s while maintaining the same other parameters caused photothrombosis of the arteriole with reperfusion in less than 1 h. This mode of photodynamic exposure caused cellular and subcellular level ischemic changes in neurons and promoted the activation of astrocytes and microglia in the first day after irradiation, but not later, without the formation of microinfarcts. This mode of photodynamic exposure most accurately reproduced human TIA, characterized by the absence of microinfarcts.

摘要

模拟人类短暂性脑缺血发作(TIA)和脑微梗死的动物模型是研究其发病机制和寻找治疗方法的重要工具。尽管单动脉光血栓形成模型具有诸多优点,但它需要复杂的实验设备和高度侵入性的手术,这可能会影响进一步研究的结果。因此,为了实现高转化潜力,我们专注于开发一种基于小动脉光血栓形成的TIA模型,以兼具良好的可重复性和低侵入性。首次使用无创激光散斑对比成像(LSCI)监测脑小动脉中的血流并实现再灌注。我们证明,在静脉注射15 mg/kg孟加拉玫瑰红后,分别使用波长532 nm、光束宽度1 mm、功率2.4或3.7 mW的激光照射小鼠大脑皮质小动脉55或40秒,会诱导相似的缺血再灌注损伤,导致微梗死形成。该模型可用于研究神经退行性疾病中自发形成的脑微梗死的发病机制。在保持其他参数不变的情况下,将照射时间缩短10秒,可使小动脉发生光血栓形成并在不到1小时内实现再灌注。这种光动力暴露模式在照射后的第一天而非之后会引起神经元细胞和亚细胞水平的缺血变化,并促进星形胶质细胞和小胶质细胞的激活,且不会形成微梗死。这种光动力暴露模式最准确地再现了以无微梗死为特征的人类TIA。

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