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A Comparative Study of Three Different Types of Stem Cells for Treatment of Rat Spinal Cord Injury

机译:三种不同类型干细胞治疗大鼠脊髓损伤的比较研究

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摘要

Three different sources of human stem cells—bone marrow-derived mesenchymal stem cells (BM-MSCs), neural progenitors (NPs) derived from immortalized spinal fetal cell line (SPC-01), and induced pluripotent stem cells (iPSCs)—were compared in the treatment of a balloon-induced spinal cord compression lesion in rats. One week after lesioning, the rats received either BM-MSCs (intrathecally) or NPs (SPC-01 cells or iPSC-NPs, both intraspinally), or saline. The rats were assessed for their locomotor skills (BBB, flat beam test, and rotarod). Morphometric analyses of spared white and gray matter, axonal sprouting, and glial scar formation, as well as qPCR and Luminex assay, were conducted to detect endogenous gene expression, while inflammatory cytokine levels were performed to evaluate the host tissue response to stem cell therapy. The highest locomotor recovery was observed in iPSC-NP-grafted animals, which also displayed the highest amount of preserved white and gray matter. Grafted iPSC-NPs and SPC-01 cells significantly increased the number of growth-associated protein 43 (GAP43+) axons, reduced astrogliosis, downregulated Casp3 expression, and increased IL-6 and IL-12 levels. hMSCs transiently decreased levels of inflammatory IL-2 and TNF-α. These findings correlate with the short survival of hMSCs, while NPs survived for 2 months and matured slowly into glia- and tissue-specific neuronal precursors. SPC-01 cells differentiated more in astroglial phenotypes with a dense structure of the implant, whereas iPSC-NPs displayed a more neuronal phenotype with a loose structure of the graft. We concluded that the BBB scores of iPSC-NP- and hMSC-injected rats were superior to the SPC-01-treated group. The iPSC-NP treatment of spinal cord injury (SCI) provided the highest recovery of locomotor function due to robust graft survival and its effect on tissue sparing, reduction of glial scarring, and increased axonal sprouting.
机译:比较了人类干细胞的三种不同来源:骨髓来源的间充质干细胞(BM-MSC),永生化脊髓胎儿细胞系(SPC-01)衍生的神经祖细胞(NP)和诱导多能干细胞(iPSC)。在治疗气球引起的大鼠脊髓压迫性病变中。损伤后一周,大鼠接受BM-MSC(鞘内)或NP(SPC-01细胞或iPSC-NP,均在脊髓内)或生理盐水。对大鼠的运动能力进行了评估(BBB,平束试验和旋转脚架)。对剩余的白和灰质,轴突发芽和神经胶质瘢痕形成进行形态计量学分析,并进行qPCR和Luminex分析,以检测内源基因的表达,同时进行炎症细胞因子水平评估宿主组织对干细胞疗法的反应。在iPSC-NP移植的动物中观察到最高的运动恢复,这也显示出最高量的保存的白和灰质。嫁接的iPSC-NP和SPC-01细胞显着增加了生长相关蛋白43(GAP43 + )轴突的数量,减少了星形胶质瘤,下调了Casp3表达,并增加了IL-6和IL-12的水平。 hMSC暂时降低了炎症性IL-2和TNF-α的水平。这些发现与hMSC的短生存期相关,而NPs可以存活2个月并缓慢成熟为神经胶质和组织特异性神经元前体。 SPC-01细胞在星形胶质表型与植入物的致密结构中分化程度更高,而iPSC-NPs在神经元表型中具有较松散的移植物结构。我们得出结论,注射iPSC-NP和hMSC的大鼠的BBB评分优于SPC-01治疗的组。 iPSC-NP治疗脊髓损伤(SCI)可提供强劲的运动功能恢复,这归因于牢固的移植物存活及其对组织保留,胶质瘢痕形成减少和轴突萌发的影响。

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