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首页> 外文期刊>Spine >Transplantation of human marrow stromal cells and mono-nuclear bone marrow cells into the injured spinal cord: a comparative study.
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Transplantation of human marrow stromal cells and mono-nuclear bone marrow cells into the injured spinal cord: a comparative study.

机译:人骨髓基质细胞和单核骨髓细胞移植到受损脊髓中的比较研究。

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摘要

STUDY DESIGN: Two groups of 6 rats received dorsolateral funiculotomies followed by direct injection of bone marrow stromal cells (MSC) or mono-nuclear fraction of bone marrow (mnBM). Animals were killed at 4 or 21 days. OBJECTIVE: Cellular transplantation is a promising treatment strategy for spinal cord injury (SCI); however, most cells need to be cultured before transplantation introducing burdensome steps for clinical application. Cells immediately available for transplantation, like mnBM, would be preferable. SUMMARY OF BACKGROUND DATA: Previous studies have shown that MSC transplants promote protection and repair after SCI. MSC are attractive for transplantation because of easy isolation and availability of autologous sources. MSC are derived from whole bone marrow, purified and expanded in culture for a period of at least 2 weeks. Alternatively, mnBM could be used for transplantation. mnBM derived from bone marrow from through simple centrifugation can be reimplantated within hours; however, the presence of immune cells may be problematic. METHODS: Cultured MSC or mnBM from human donors were acutely transplanted into SCI. After sacrifice, spinal cord sections were histologically analyzed for presence of graft-derived immune cells, host immune response, tissue sparing, glial scar formation, and grafting efficacy. RESULTS: mnBM did not give rise to mature immune cells after transplantation into SCI, or evoke an increased host immune response or tissue loss compared to MSC-transplanted animals. In contrast, host macrophage/microglia response was increased early after MSC transplantation, perhaps due to exposure of cells to serum-containing media. The glial scar was less prominent after mnBM transplantation at day 4. At 21 days, differences had subsided and MSC and mnBM macrophage responses and effects on glial scarring were comparable. MSC and mnBM engraftment efficiencies were also similar. CONCLUSION: The use of mnBM is a viable alternative to MSC for transplantation into SCI and may dramatically ease clinical translation.
机译:研究设计:两组,每只6只大鼠接受背外侧功能治疗,然后直接注射骨髓基质细胞(MSC)或骨髓单核级分(mnBM)。在4或21天处死动物。目的:细胞移植是一种有希望的脊髓损伤(SCI)治疗策略。然而,大多数细胞需要在移植前进行培养,为临床应用带来繁重的步骤。立即可用于移植的细胞(如mnBM)会更好。背景数据概述:先前的研究表明,MSC移植促进SCI后的保护和修复。 MSC由于易于分离和自体来源的可用性而吸引了移植。 MSC来源于整个骨髓,经过纯化和培养至少2周。另外,mnBM可用于移植。通过简单离心获得的源自骨髓的mnBM可在数小时内重新植入;然而,免疫细胞的存在可能是有问题的。方法:将来自人类供体的培养的MSC或mnBM急性移植到SCI中。处死后,对脊髓切片进行组织学分析,以确定是否存在源自移植物的免疫细胞,宿主免疫反应,组织节约,神经胶质瘢痕形成和移植功效。结果:与MSC移植的动物相比,mnBM移植到SCI后没有产生成熟的免疫细胞,也没有引起宿主免疫反应增强或组织损失。相反,MSC移植后宿主巨噬细胞/小胶质细胞反应增加,可能是由于细胞暴露于含血清的培养基中。在第4天进行mnBM移植后,神经胶质瘢痕不那么明显。在21天时,差异已经消退,MSC和mnBM巨噬细胞反应和对神经胶质瘢痕形成的影响相当。 MSC和mnBM的植入效率也相似。结论:mnBM可以替代MSC移植到SCI中,并且可以大大简化临床翻译。

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