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Comparison of the therapeutic effects of bone marrow mononuclear cells and microglia for permanent cerebral ischemia

机译:骨髓单个核细胞和小胶质细胞治疗永久性脑缺血的疗效比较

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摘要

In this study we transplanted bone marrow mononuclear cells (BM-MNCs) or microglia into rats that had undergone permanent cerebral ischemia and observed the distribution or morphology of transplanted cells in vivo. In addition, we also compared the effects of BM-MNCs and microglia on infarct volume, brain water content, and functional outcome after permanent cerebral ischemia. BM-MNCs and microglia were obtained from femur and brain, respectively, of newborn rats. Adult rats were injected with vehicle or 3 million BM-MNCs or microglia via the tail vein 24 h after permanent middle cerebral artery occlusion (pMCAO). The distribution or morphologic characteristics of transplanted BM-MNCs (BrdU/double-stained CD34 and CD45) and microglia (BrdU/double-stained Iba-1) were detected with immunofluorescent staining at 3 or 7 and 14 days after pMCAO. Functional deficits were assessed by the modified neurologic severity score at 1, 3, 7 and 14 days after pMCAO. Brain water content was assessed with dry–wet weight method at 3 days, and infarct volume was determined with 2,3,5-triphenyltetrazolium chloride (TTC) staining at 14 days. More BrdU/double-stained CD45- and Iba-1-positive cells were observed than BrdU/double-stained CD34-positive cells around the infarcted area. Some infused microglia show the morphology of innate microglia at 7 days and the increased numbers can be detected at 14 days after pMCAO. BM-MNC-treated rats showed a significant reduction in infarct volume and brain water content compared to vehicle- and microglia-treated rats. In addition, BM-MNC treatment reduced neurologic deficit scores compared to those in the other groups. The results provide evidence that infusion of BM-MNC, but not microglia, is neuroprotective after permanent cerebral ischemia.
机译:在这项研究中,我们将骨髓单核细胞(BM-MNCs)或小胶质细胞移植到经历了永久性脑缺血的大鼠中,并观察了体内移植细胞的分布或形态。此外,我们还比较了BM-MNC和小胶质细胞对永久性脑缺血后梗死体积,脑含水量和功能结局的影响。 BM-MNC和小胶质细胞分别来自新生大鼠的股骨和大脑。成年大鼠在永久性大脑中动脉闭塞(pMCAO)后24小时通过尾静脉注射了媒介物或300万个BM-MNC或小胶质细胞。在pMCAO后3、7和14天通过免疫荧光染色检测移植的BM-MNCs(BrdU /双重染色的CD34和CD45)和小胶质细胞(BrdU /双重染色的Iba-1)的分布或形态特征。通过在pMCAO后1、3、7和14天的改良神经系统严重程度评分评估功能障碍。在第3天用干湿重法评估脑水含量,在第14天用2,3,5-三苯基四唑氯化物(TTC)染色确定梗塞体积。在梗塞区域周围观察到比BrdU /双重染色的CD34阳性细胞更多的BrdU /双重染色的CD45和Iba-1阳性细胞。一些注入的小胶质细胞在7天时表现出先天性小胶质细胞的形态,并且在pMCAO后14天可以检测到数量增加。与用媒介物和小胶质细胞治疗的大鼠相比,用BM-MNC治疗的大鼠显示梗塞体积和脑含水量显着减少。此外,与其他组相比,BM-MNC治疗降低了神经功能缺损评分。该结果提供了证据,证实永久性脑缺血后注入BM-MNC而非小胶质细胞具有神经保护作用。

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