Delayed cerebral ischemia (DCI) is a significant cause of morbidity and mortality for patients surviving the rupture of an intracranial aneurysm. Despite an association between vasospasm and DCI, thrombosis and thromboembolism may also contribute to DCI. In this study we investigate the time course of intravascular microclot formation after experimental subarachnoid hemorrhage (SAH) and assess the effects of the following two drugs on microclot burden: mutant thrombin-activated urokinase-type plasminogen activator (scFv/uPA-T), which is bound to red blood cells for use as a thromboprophylactic agent, and clazosentan, an endothelin antagonist. In the first study, adult male C57BL/6 mice were sacrificed at 24 (n=5), 48 (n=6), 72 (n=8), and 96 (n=3) hours after SAH induced by filament perforation of the anterior cerebral artery. Sham animals (n=5) underwent filament insertion without puncture. In the second study, animals received scFv/uPA-T (n=5) 3 hours after hemorrhage, clazosentan (n=5) by bolus and subcutaneous pump after SAH just prior to skin closure, or a combination of scFv/uPA-T and clazosentan (n=4). Control (n=6) and sham (n=5) animals received saline alone. All animals were sacrificed at 48 hours and underwent intra-cardiac perfusion with 4% paraformaldehyde. The brains were then extracted and sliced coronally on a cryostat and processed for immunohistochemistry. An antibody recognizing thrombin–anti-thrombin complexes was used to detect microclots on coronal slices. Microclot burden was calculated for each animal and compared among groups. Following SAH, positive anti-thrombin staining was detected bilaterally in the following brain regions, in order of decreasing frequency: cortex; hippocampus; hypothalamus; basal ganglia. Few microclots were found in the shams. Microclot burden peaked at 48 hours and then decreased gradually. Animals receiving scFv/uPA-T and scFv/uPA-T+clazosentan had a lower microclot burden than controls, whereas animals receiving clazosentan alone had a higher microclot burden (p<0.005). The overall mortality rate in the time course study was 40%; mortality was highest among control animals in the second study. Intravascular microclots form in a delayed fashion after experimental SAH. Microclots may be safely reduced using a novel form of thromboprophylaxis provided by RBC-targeted scFv/uPA-T and represent a potential target for therapeutic intervention in the treatment of DCI.
The idea of using 3D point clouds obtained with the aid of a handheld 3D laser scanner for the quality assurance of high-frequency mechanical impact (HFMI) treatment is proposed and demonstrated in this paper. The effectiveness of impact treatments for extending the fatigue lives of welded structures has been demonstrated in numerous studies. Guidelines for the proper execution of impact treatments have been developed. A lack of suitable quality assurance (QA) procedures for accepting or rejecting the treatment after completion has been previously identified. In contrast with the existing QA procedures, which are based mainly on controlling inputs and visual inspection, a technology-based, quantitative methodology is developed in this paper. Five welded specimens were subjected to impact treatment at various levels to simulate under-, proper, and over-treatment. A handheld 3D laser scanner was then used to facilitate a point cloud-based method to determine the geometric parameters of the treated weld toe groove, which were then measured manually. The results show that the proposed methodology is successful in identifying the different treatment levels. This approach has a number of advantages over the existing QA methods, including the following: providing quantitative measures, ease of use, and archive-ability.
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