首页> 美国卫生研究院文献>The Journal of Neuroscience >Intravenous Transplants of Human Adipose-Derived Stem Cell Protect the Brain from Traumatic Brain Injury-Induced Neurodegeneration and Motor and Cognitive Impairments: Cell Graft Biodistribution and Soluble Factors in Young and Aged Rats
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Intravenous Transplants of Human Adipose-Derived Stem Cell Protect the Brain from Traumatic Brain Injury-Induced Neurodegeneration and Motor and Cognitive Impairments: Cell Graft Biodistribution and Soluble Factors in Young and Aged Rats

机译:人脂肪干细胞的静脉移植可保护大脑免受创伤性脑损伤诱导的神经变性以及运动和认知障碍的影响:年轻和成年大鼠的细胞移植物生物分布和可溶性因子

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摘要

Traumatic brain injury (TBI) survivors exhibit motor and cognitive symptoms from the primary injury that can become aggravated over time because of secondary cell death. In the present in vivo study, we examined the beneficial effects of human adipose-derived stem cells (hADSCs) in a controlled cortical impact model of mild TBI using young (6 months) and aged (20 months) F344 rats. Animals were transplanted intravenously with 4 × 106 hADSCs (Tx), conditioned media (CM), or vehicle (unconditioned media) at 3 h after TBI. Significant amelioration of motor and cognitive functions was revealed in young, but not aged, Tx and CM groups. Fluorescent imaging in vivo and ex vivo revealed 1,1′ dioactadecyl-3-3-3′,3′-tetramethylindotricarbocyanine iodide-labeled hADSCs in peripheral organs and brain after TBI. Spatiotemporal deposition of hADSCs differed between young and aged rats, most notably reduced migration to the aged spleen. Significant reduction in cortical damage and hippocampal cell loss was observed in both Tx and CM groups in young rats, whereas less neuroprotection was detected in the aged rats and mainly in the Tx group but not the CM group. CM harvested from hADSCs with silencing of either NEAT1 (nuclear enriched abundant transcript 1) or MALAT1 (metastasis associated lung adenocarcinoma transcript 1), long noncoding RNAs (lncRNAs) known to play a role in gene expression, lost the efficacy in our model. Altogether, hADSCs are promising therapeutic cells for TBI, and lncRNAs in the secretome is an important mechanism of cell therapy. Furthermore, hADSCs showed reduced efficacy in aged rats, which may in part result from decreased homing of the cells to the spleen.
机译:颅脑外伤(TBI)幸存者表现出原发性损伤的运动和认知症状,由于继发性细胞死亡,随着时间的流逝,这些症状可能会加重。在目前的体内研究中,我们在年轻(6个月)和年龄(20个月)的F344大鼠中,研究了人脂肪衍生干细胞(hADSCs)在轻度TBI对照皮层撞击模型中的有益作用。在TBI后3小时,将动物用4×10 6 hADSCs(Tx),条件培养基(CM)或媒介物(非条件培养基)静脉内移植。 Tx和CM的年轻群体(而非老年群体)显示出明显的运动和认知功能改善。体内和离体的荧光成像显示TBI后外周器官和大脑中1,1'十二内酯基-3-3-3',3'-四甲基吲哚并花青素碘标记的hADSCs。 hADSCs的时空沉积在幼鼠和老年大鼠之间有所不同,最明显的是减少了向老年脾脏的迁移。在年轻大鼠的Tx和CM组中均观察到皮质损伤和海马细胞损失显着减少,而在老年大鼠中检测到的神经保护作用较少,并且主要在Tx组但未在CM组中。从hADSCs收获的CM带有NEAT1(富含核的丰富转录本1)或MALAT1(与转移有关的肺腺癌转录本1)沉默,而长的非编码RNA(lncRNA)已知在基因表达中起作用,在我们的模型中失去了功效。总的来说,hADSCs是有希望的TBI治疗细胞,而分泌组中的lncRNAs是细胞治疗的重要机制。此外,hADSCs在衰老大鼠中显示出降低的功效,这可能部分归因于细胞归巢至脾脏的减少。

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