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G-CSF and hypoxic conditioning improve the proliferation, neural differentiation and migration of canine bone marrow mesenchymal stem cells

机译:G-CSF和缺氧条件改善了犬骨髓间充质干细胞的增殖,神经分化和迁移

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摘要

Transplantation using bone marrow mesenchymal stem cells (BMSCs) is emerging as a potential regenerative therapy after ischemic attacks in the brain. However, it has been questioned because very few transplanted BMSCs are detected homing to and survived in the ischemic region. Improving the cell viability and migration ability under the complex ischemic condition seems very important. The aim of our study is to identify whether hypoxic condition and granulocyte colony-stimulating factor (G-CSF) could improve the cell survival and migration ability of transplanted cells or hypoxic condition could promote BMSC's neural differentiation. BMSCs were treated under either normoxic (21% O-2) or hypoxic (1% O-2) (HP-BMSCs) conditions, no significant apoptosis was observed in hypoxic precondition (HP) group, our study confirmed that HP improves BMSCs proliferation and migration. Meanwhile, neural induction of BMSCs under hypoxic condition exhibited significant superior results than normoxic condition. Additionally, the addition of G-CSF in HP-BMSCs culture media promoted HP efficiency on BMSCs. These findings shed light on novel efficient strategy on the prosperity of BMSCs. Hypoxic preconditioning and cultured with G-CSF may become a promising therapeutics for cell-based therapy in the treatments of ischemia stroke.
机译:在大脑缺血发作后,使用骨髓间充质干细胞(BMSC)进行的移植正在成为一种潜在的再生疗法。然而,由于几乎没有检测到移植的BMSC归巢于缺血区域并在缺血区域存活而受到质疑。在复杂的缺血条件下提高细胞活力和迁移能力似乎非常重要。我们的研究目的是确定低氧条件和粒细胞集落刺激因子(G-CSF)是否可以提高移植细胞的存活率和迁移能力,或者低氧条件是否可以促进BMSC的神经分化。在常氧(21%O-2)或低氧(1%O-2)(HP-BMSCs)条件下处理BMSCs,在低氧预处理(HP)组中未观察到明显的细胞凋亡,我们的研究证实HP可改善BMSCs的增殖和迁移。同时,在缺氧条件下对BMSCs的神经诱导表现出比常氧条件下明显更好的结果。此外,在HP-BMSCs培养基中添加G-CSF可以提高HP在BMSCs上的效率。这些发现为BMSCs的繁荣提供了新的有效策略。缺氧预处理并与G-CSF一起培养可能成为基于细胞的缺血性卒中治疗的有前途的治疗方法。

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