首页> 外文期刊>Biochemical and Biophysical Research Communications >Transplanted neural progenitor cells expressing mutant NT3 promote myelination and partial hindlimb recovery in the chronic phase after spinal cord injury.
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Transplanted neural progenitor cells expressing mutant NT3 promote myelination and partial hindlimb recovery in the chronic phase after spinal cord injury.

机译:表达突变型NT3的移植神经祖细胞在脊髓损伤后的慢性期促进髓鞘形成和部分后肢恢复。

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摘要

Neutrotrophin-3 (NT3) plays a protective role in injured central nervous system tissues through interaction with trk receptors. To enhance the regeneration of damaged tissue, a combination therapy with cell transplantation and neurotrophins has been under development. We examined whether the transplantation of neural progenitor cells (NPCs) secreting NT3/D15A, a multi-neurotrophin with the capacity to bind both trkB and trkC, would enhance the repair of damaged tissues and the functional recovery in a chronic phase of spinal cord injury. The cultured NPCs with lentiviral vector containing either GFP or NT3/D15A were transplanted into the contused spinal cord at 6 weeks after the initial thoracic injury. Eight weeks after the transplantation, the NT3/D15A transplants displayed better survival than the GFP transplants, and they exhibited enhanced myelin formation and partial improvement of hindlimb function. Our study revealed that NT3/D15A produced positive effects in injured spinal cords even in the chronic phase. These effects suggest an enhanced neurotrophin-trk signaling by NT3/D15A.
机译:Neutrotrophin-3(NT3)通过与trk受体的相互作用在受伤的中枢神经系统组织中发挥保护作用。为了增强受损组织的再生,已经在开发与细胞移植和神经营养蛋白的组合疗法。我们检查了分泌NT3 / D15A(一种具有结合trkB和trkC的能力的多神经营养蛋白)的神经祖细胞(NPC)的移植是否会在脊髓损伤的慢性期增强受损组织的修复和功能恢复。在最初的胸腔损伤后第6周,将含有慢病毒载体的含有GFP或NT3 / D15A的培养NPC移植到挫伤的脊髓中。移植后八周,NT3 / D15A移植的存活率优于GFP移植,并且髓鞘形成增强,后肢功能得到部分改善。我们的研究表明,即使在慢性期,NT3 / D15A也会在受伤的脊髓中产生积极作用。这些作用表明NT3 / D15A增强了神经营养蛋白-trk信号。

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