首页> 外文期刊>Journal of Neuroscience Research >Matrigel supports survival and neuronal differentiation of grafted embryonic stem cell-derived neural precursor cells.
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Matrigel supports survival and neuronal differentiation of grafted embryonic stem cell-derived neural precursor cells.

机译:基质胶支持移植的胚胎干细胞来源的神经前体细胞的存活和神经元分化。

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Cell replacement therapy holds great promise as a means of treating neurological disorders, including Parkinson's disease. However, one of the major obstacles to the success of this treatment is the low survival rate of grafted cells, which probably results from mechanical damage, acute inflammation, and immunological rejection. To overcome this problem, we investigated the effect of different types of extracellular matrix (ECM) on the survival and differentiation of embryonic stem (ES) cell-derived neural precursor cells (NPCs). We tested materials from natural sources, including collagen, ornithine/laminin, and growth factor-reduced Matrigel (gfrMG), as well as the synthetic biomaterial PuraMatrix, which consists of self-assembling polypeptides. GfrMG efficiently supported cell survival, migration, and neurite outgrowth in vitro and promoted proliferation of grafted cells in vivo, resulting in larger graft volume and an increase in the number of TH-positive dopaminergic neurons in the graft. GfrMG did not induce dopaminergic differentiation directly; rather, it reduced the invasion of pan-leukocytic CD45-positive cells into the graft. Insofar as the inflammatory or immune response in the host brain inhibits neuronal differentiation of grafted NPCs, gfrMG may increase the number of TH-positive cells by suppressing this effect. Thus, gfrMG appears to provide a suitable scaffold that supports survival and differentiation of NPCs. However, because it is derived from mouse sarcomas, a human-derived matrix or synthetic biomaterial must be developed for clinical applications.
机译:细胞替代疗法有望作为治疗包括帕金森氏症在内的神经系统疾病的一种手段。然而,该治疗成功的主要障碍之一是移植细胞的低存活率,这可能是由于机械损伤,急性炎症和免疫排斥引起的。为克服此问题,我们研究了不同类型的细胞外基质(ECM)对源自胚胎干(ES)细胞的神经前体细胞(NPC)存活和分化的影响。我们测试了天然来源的材料,包括胶原蛋白,鸟氨酸/层粘连蛋白和生长因子减少型基质胶(gfrMG),以及由自组装多肽组成的合成生物材料PuraMatrix。 GfrMG在体外有效地支持细胞存活,迁移和神经突生长,并在体内促进移植细胞的增殖,从而导致更大的移植物体积和移植物中TH阳性多巴胺能神经元的数量增加。 GfrMG没有直接诱导多巴胺能分化。相反,它减少了泛白细胞CD45阳性细胞向移植物中的侵袭。只要宿主脑中的炎症或免疫反应抑制了移植NPC的神经元分化,gfrMG可能会通过抑制这种作用来增加TH阳性细胞的数量。因此,gfrMG似乎提供了支持NPC存活和分化的合适支架。但是,由于它源自小鼠肉瘤,因此必须开发人源性基质或合成生物材料以用于临床应用。

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