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首页> 外文期刊>BMC Neuroscience >Transplanted bone marrow stem cells relocate to infarct penumbra and co-express endogenous proliferative and immature neuronal markers in a mouse model of ischemic cerebral stroke
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Transplanted bone marrow stem cells relocate to infarct penumbra and co-express endogenous proliferative and immature neuronal markers in a mouse model of ischemic cerebral stroke

机译:移植的骨髓干细胞迁移到梗死的半影和共同表达内源性增殖和未成熟的神经元标志物中的缺血性脑卒中的小鼠模型

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Background Several studies demonstrate that neurogenesis may be induced or activated following vascular insults, which may be important for neuronal regeneration and functional recovery. Understanding the cellular mechanism underlying stroke-associated neurogenesis is of neurobiological as well as neurological/clinical relevance. The present study attempted to explore potential homing and early development of transplanted bone marrow stem cells in mouse forebrain after focal occlusion of the middle cerebral artery, an experimental model of ischemic stroke. Results Bone marrow stem cells isolated from donor mice were confirmed by analysis of surface antigen profile, and were pre-labeled with a lipophilic fluorescent dye PKH26, and subsequently transfused into recipient mice with middle cerebral artery coagulation. A large number of PKH26-labeled cells were detected surrounding the infarct site, most of which colocalized with immunolabelings for the proliferating cell nuclear antigen (PCNA) and some also colocalized with the immature neuronal marker doublecortin (DCX) during 1-2 weeks after the bone marrow cells transfusion. Conclusions The present study shows that transplanted bone morrow cells largely relocate to the infarct penumbra in ischemic mouse cerebrum. These transplanted bone marrow cells appear to undergo a process of in situ proliferation and develop into putative cortical interneurons during the early phase of experimental vascular injury.
机译:背景技术几项研究表明,在血管损伤后可以诱导或激活神经发生,这对于神经元再生和功能性回收可能是重要的。理解潜在的中风相关神经发生的细胞机制是神经生物学以及神经学/临床相关性。本研究试图探讨在脑动脉局灶性闭塞后小鼠前脑中移植骨髓干细胞的潜在归巢和早期发育,缺血性卒中的实验模型。结果通过表面抗原型分析证实了从供体小鼠中分离的骨髓干细胞,并用亲脂荧光染料PKH 26预先标记,随后用中间脑动脉凝固转移到受体小鼠中。围绕梗塞部位检测大量pKH26标记的细胞,其中大部分是用免疫标记分致用于增殖细胞核抗原(PCNA)的分致统一,并且在1-2周后,其中一些也与未成熟的神经元标记物(DCX)结合骨髓细胞输血。结论本研究表明,移植的骨假细胞在很大程度上迁移到缺血小鼠大脑中的梗塞半影。这些移植的骨髓细胞似乎在实验血管损伤的早期阶段发生原位增殖并发展到推定的皮质型细胞核。

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