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微梗死大鼠模型血脑屏障破坏后血管周围血液蛋白清除。

Perivascular clearance of blood proteins after blood-brain barrier disruption in a rat model of microinfarcts.

机构信息

Amsterdam UMC Location University of Amsterdam, Biomedical Engineering and Physics, Meibergdreef 9, Amsterdam, the Netherlands.

Amsterdam UMC Location University of Amsterdam, Biomedical Engineering and Physics, Meibergdreef 9, Amsterdam, the Netherlands; Amsterdam Cardiovascular Sciences, Microcirculation, Amsterdam, the Netherlands.

出版信息

Microvasc Res. 2023 Jul;148:104515. doi: 10.1016/j.mvr.2023.104515. Epub 2023 Mar 7.

Abstract

Microinfarcts result in a transient loss of the blood-brain barrier (BBB) in the ischemic territory. This leads to the extravasation of blood proteins into the brain parenchyma. It is not clear how these proteins are removed. Here we studied the role of perivascular spaces in brain clearance from extravasated blood proteins. Male and female Wistar rats were infused with microspheres of either 15, 25, or 50 μm in diameter (n = 6 rats per group) via the left carotid artery. We infused either 25,000 microspheres of 15 μm, 5500 of 25 μm, or 1000 of 50 μm. One day later, rats were infused with lectin and hypoxyprobe to label perfused blood vessels and hypoxic areas, respectively. Rats were then euthanized and perfusion-fixed. Brains were excised, sectioned, and analyzed using immunostaining and confocal imaging. Microspheres induced a size-dependent increase in ischemic volume per territory, but the cumulative ischemic volume was similar in all groups. The total volumes of ischemia, hypoxia and infarction affected 1-2 % of the left hemisphere. Immunoglobulins (IgG) were present in ischemic brain tissue surrounding lodged microspheres in all groups. In addition, staining for IgG was found in perivascular spaces of blood vessels nearby areas of BBB disruption. About 2/3 of these vessels were arteries, while the remaining 1/3 of these vessels were veins. The subarachnoid space (SAS) of the affected hemisphere stained stronger for IgG than the contralateral hemisphere in all groups: +27 %, +44 % and +27 % respectively. Microspheres of various sizes induce a local loss of BBB integrity, evidenced by parenchymal IgG staining. The presence of IgG in perivascular spaces of both arteries and veins distinct from the ischemic territories suggests that both contribute to the removal of blood proteins. The strong staining for IgG in the SAS of the affected hemisphere suggests that this perivascular route egresses via the CSF. Perivascular spaces therefore play a previously unrecognized role in tissue clearance of fluid and extravasated proteins after BBB disruption induced by microinfarcts.

摘要

微梗死导致缺血区域的血脑屏障(BBB)短暂丧失。这导致血液蛋白渗出到脑实质中。目前尚不清楚这些蛋白质是如何被清除的。在这里,我们研究了血管周围空间在清除渗出的血液蛋白中的作用。雄性和雌性 Wistar 大鼠通过左侧颈总动脉输注直径为 15、25 或 50 μm 的微球(每组 6 只大鼠)。我们分别输注了 25,000 个 15 μm 的微球、5500 个 25 μm 的微球或 1000 个 50 μm 的微球。一天后,大鼠分别用凝集素和缺氧探针标记灌注血管和缺氧区域。然后处死大鼠并进行灌注固定。取出大脑,切片,并用免疫染色和共聚焦成像进行分析。微球诱导的每个区域的缺血体积呈大小依赖性增加,但所有组的累积缺血体积相似。缺血、缺氧和梗死的总体积影响左半球的 1-2%。所有组的缺血脑组织中均存在免疫球蛋白(IgG)。此外,在 BBB 破坏附近区域的血管周围空间中也发现了 IgG 染色。这些血管中约有 2/3 为动脉,其余 1/3 为静脉。受影响半球的蛛网膜下腔(SAS)比所有组的对侧半球对 IgG 的染色更强:分别为+27%、+44%和+27%。各种大小的微球诱导局部 BBB 完整性丧失,这表现为实质 IgG 染色。在与缺血区域不同的动静脉血管周围空间中存在 IgG,表明两者都有助于清除血液蛋白。受影响半球的 SAS 中 IgG 的强烈染色表明,这种血管周围途径通过 CSF 排出。因此,血管周围空间在微梗死引起的 BBB 破坏后,对组织清除液体和渗出蛋白起着以前未被认识的作用。

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