首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >Escape of intraluminal platelets into brain parenchyma after subarachnoid hemorrhage.
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Escape of intraluminal platelets into brain parenchyma after subarachnoid hemorrhage.

机译:蛛网膜下腔出血后腔内血小板逸出进入脑实质。

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摘要

Platelet aggregates are present in parenchymal vessels as early as 10 min after experimental subarachnoid hemorrhage (SAH). Structural injury to parenchymal vessel walls and depletion of collagen-IV (the major protein of basal lamina) occur in a similar time frame. Since platelets upon activation release enzymes which can digest collagen-IV, we investigated the topographic relationship between platelet aggregates, endothelium, and basal lamina after SAH produced by endovascular perforation, using triple immunofluorescence and confocal microscopy with deconvolution. The location of platelet aggregates in relation to zymography-detected active collagenase was also examined. As reported previously, most cerebral vessels profiles contained platelets aggregates at 10 min after SAH. High-resolution three-dimensional image analysis placed many platelets at the ab-luminal (basal) side of endothelium at 10 min, and others either within the vascular basal lamina or in nearby parenchyma. By 24 h post hemorrhage, large numbers of platelets had entered the brain parenchyma. The vascular sites of platelet movement were devoid of endothelium and collagen-IV. Collagenase activity colocalized with vascular platelet aggregates. Our data demonstrate that parenchymal entry of platelets into brain parenchyma begins within minutes after hemorrhage. Three-dimensional analysis suggests that platelet aggregates initiate or stimulate local disruption of endothelium and destruction of adjacent basal lamina after SAH.
机译:实验性蛛网膜下腔出血(SAH)后10分钟,血小板聚集体就存在于实质性血管中。实质性血管壁的结构性损伤和IV型胶原(基底层的主要蛋白)的耗竭在相似的时间范围内发生。由于活化后的血小板释放可消化胶原IV的酶,因此我们使用三重免疫荧光和共聚焦显微镜与反褶积技术研究了血管内穿孔产生的SAH后血小板聚集体,内皮和基底层之间的形貌关系。还检查了血小板聚集体相对于酶法检测到的活性胶原酶的位置。如先前报道,大多数脑血管图谱显示SAH后10分钟时血小板聚集。高分辨率三维图像分析在10分钟时将许多血小板放置在内皮的ab-腔(基底)侧,其他则放置在血管基底层或附近的薄壁组织中。出血后24小时,大量血小板进入脑实质。血小板运动的血管部位没有内皮和IV型胶原。胶原酶活性与血管血小板聚集物共定位。我们的数据表明,血小板实质进入出血后几分钟内就开始进入脑实质。三维分析表明,SAH后血小板聚集体启动或刺激内皮的局部破坏以及相邻基底层的破坏。

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