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自体猪骨髓单个核细胞向功能性许旺细胞表型的诱导分化及其在神经修复中的作用。

Development of a functional schwann cell phenotype from autologous porcine bone marrow mononuclear cells for nerve repair.

机构信息

Providence Health and Services, 9555 SW Barnes Rd., Portland, OR 97225, USA.

出版信息

Stem Cells Int. 2012;2012:738484. doi: 10.1155/2012/738484. Epub 2012 Jun 24.

Abstract

Adult bone marrow mononuclear cells (BM-MNCs) are a potential resource for making Schwann cells to repair damaged peripheral nerves. However, many methods of producing Schwann-like cells can be laborious with the cells lacking a functional phenotype. The objective of this study was to develop a simple and rapid method using autologous BM-MNCs to produce a phenotypic and functional Schwann-like cell. Adult porcine bone marrow was collected and enriched for BM-MNCs using a SEPAX device, then cells cultured in Neurobasal media, 4 mM L-glutamine and 20% serum. After 6-8 days, the cultures expressed Schwann cell markers, S-100, O4, GFAP, were FluoroMyelin positive, but had low p75(NGF) expression. Addition of neuregulin (1-25 nM) increased p75(NGF) levels at 24-48 hrs. We found ATP dose-dependently increased intracellular calcium Ca(2+), with nucleotide potency being UTP = ATP > ADP > AMP > adenosine. Suramin blocked the ATP-induced Ca(2+) but α, β,-methylene-ATP had little effect suggesting an ATP purinergic P2Y2 G-protein-coupled receptor is present. Both the Schwann cell markers and ATP-induced Ca(2+) sensitivity decreased in cells passaged >20 times. Our studies indicate that autologous BM-MNCs can be induced to form a phenotypic and functional Schwann-like cell which could be used for peripheral nerve repair.

摘要

成人骨髓单核细胞(BM-MNCs)是产生施万细胞以修复受损周围神经的潜在资源。然而,许多产生类施万细胞的方法都很繁琐,而且细胞缺乏功能表型。本研究的目的是开发一种使用自体 BM-MNCs 产生具有表型和功能的类施万细胞的简单快速方法。采集成年猪骨髓,使用 SEPAX 设备富集 BM-MNCs,然后在含有 4mM L-谷氨酰胺和 20%血清的 Neurobasal 培养基中培养细胞。培养 6-8 天后,细胞表达施万细胞标志物 S-100、O4、GFAP,FluoroMyelin 阳性,但 p75(NGF)表达水平较低。添加神经调节蛋白(1-25 nM)可在 24-48 小时内增加 p75(NGF)水平。我们发现 ATP 剂量依赖性地增加细胞内钙离子浓度Ca(2+),核苷酸效力为 UTP = ATP > ADP > AMP > 腺苷。苏拉明阻断 ATP 诱导的Ca(2+),但α、β-亚甲基-ATP 影响较小,提示存在 ATP 嘌呤能 P2Y2 G 蛋白偶联受体。随着细胞传代超过 20 次,施万细胞标志物和 ATP 诱导的Ca(2+)敏感性均降低。我们的研究表明,自体 BM-MNCs 可被诱导形成具有表型和功能的类施万细胞,可用于周围神经修复。

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