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首页> 外文期刊>NMR in biomedicine >MRI assessment of the intra-carotid route for macrophage delivery after transient cerebral ischemia
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MRI assessment of the intra-carotid route for macrophage delivery after transient cerebral ischemia

机译:短暂性脑缺血后颈动脉内巨噬细胞递送途径的MRI评估

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The broad aim underlying the present research was to investigate the distribution and homing of bone marrow-derived macrophages in a rodent model of transient middle cerebral artery occlusion usingMRI and ultrasmall superparamagnetic iron oxide (USPIO) to magnetically label bone marrow-derived macrophages. The specific aim was to assess the intra-carotid infusion route for bone marrow-derived macrophage delivery at reperfusion. Fifteen Sprague–Dawley rats sustained 1 h of middle cerebral artery occlusion. USPIO-labeled bone marrow-derived macrophages were slowly injected for 5 min immediately after reperfusion in ischemic animals (n = 7), 1 h after the end of surgery in sham animals (n = 5) and very shortly after anesthesia in healthy animals (n = 3). Multiparametric MRI was performed at day 0, just after cell administration, and repeated at day 1. Immunohistological analysis included Prussian blue for iron detection and rat endothelial cell antigen-1 for endothelium visualization. Intra-carotid cell delivery brought a large number of cells to the ipsilateral hemisphere of the brain, as seen on both MRI and immunohistology. However, it was associated with high mortality (50%). The study of sham animals demonstrated that intra-carotid cell delivery could induce ischemic lesions and may thus favor additional brain damage. The present study highlights severe drawbacks to the intra-carotid delivery of macrophages at the time of reperfusion in this rodent model of transient cerebral ischemia. Multiparametric MRI appears to be a method of choice to monitor longitudinally the effects of cell infusion, allowing the assessment of both cell fate with the help of magnetic labeling and of potential tissue damage.
机译:本研究的广泛目标是利用MRI和超小型超顺磁性氧化铁(USPIO)磁性标记骨髓源性巨噬细胞,研究短暂性大脑中动脉阻塞的啮齿动物模型中骨髓源性巨噬细胞的分布和归巢。具体目的是评估在再灌注时颈内输注途径用于骨髓源性巨噬细胞的递送。十五只Sprague–Dawley大鼠持续1 h大脑中动脉闭塞。在缺血动物(n = 7)再灌注后,假手术动物(n = 5)手术结束后1小时以及健康动物(麻醉后)不久之后,立即将USPIO标记的骨髓巨噬细胞缓慢注射5分钟。 n = 3)。多参数MRI在细胞给药后第0天进行,并在第1天重复进行。免疫组织学分析包括普鲁士蓝用于铁检测,大鼠内皮细胞抗原-1用于内皮显像。 MRI和免疫组织学均显示,颈动脉内细胞递送将大量细胞带入大脑的同侧半球。但是,它与高死亡率(50%)有关。对假动物的研究表明,颈动脉内的细胞递送可以诱导缺血性损伤,因此可能会增加脑损伤。本研究突出了在这种短暂性脑缺血的啮齿动物模型中,再灌注时巨噬细胞颈动脉内递送的严重缺陷。多参数MRI似乎是纵向监测细胞输注效果的一种选择方法,可以借助磁性标记和潜在的组织损伤来评估细胞命运。

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