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Nanotransfection-based vasculogenic cell reprogramming drives functional recovery in a mouse model of ischemic stroke

机译:基于纳米转染的血管基细胞重编程驱动缺血性卒中小鼠模型中的功能恢复

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摘要

Ischemic stroke causes vascular and neuronal tissue deficiencies that could lead to substantial functional impairment and/or death. Although progenitor-based vasculogenic cell therapies have shown promise as a potential rescue strategy following ischemic stroke, current approaches face major hurdles. Here, we used fibroblasts nanotransfected with Etv2 , Foxc2 , and Fli1 ( EFF ) to drive reprogramming-based vasculogenesis, intracranially, as a potential therapy for ischemic stroke. Perfusion analyses suggest that intracranial delivery of EFF -nanotransfected fibroblasts led to a dose-dependent increase in perfusion 14 days after injection. MRI and behavioral tests revealed ~70% infarct resolution and up to ~90% motor recovery for mice treated with EFF -nanotransfected fibroblasts. Immunohistological analysis confirmed increases in vascularity and neuronal cellularity, as well as reduced glial scar formation in response to treatment with EFF -nanotransfected fibroblasts. Together, our results suggest that vasculogenic cell therapies based on nanotransfection-driven (i.e., nonviral) cellular reprogramming represent a promising strategy for the treatment of ischemic stroke.
机译:缺血性卒中导致血管和神经元组织缺陷,可能导致具有实质性损伤和/或死亡。虽然基于祖母血管原性细胞疗法表现出承诺作为缺血性卒中后潜在的救援战略,但目前的方法面临着主要障碍。在此,我们使用用EtV2,FoxC2和FLI1(EFF)的成纤维细胞纳米转染,以使颅内转向基于重编程的血管生成,作为缺血性卒中的潜在疗法。灌注分析表明Eff-Nanotransfected成纤维细胞的颅内递送导致注射后14天的灌注剂量依赖性增加。 MRI和行为试验揭示了用EFF-Nanotransfected成纤维细胞处理的小鼠的梗塞分辨率〜70%的梗塞分辨率和高达约90%的电动机恢复。免疫组织学分析证实血管性和神经元细胞性的增加,以及响应于用Eff-Nanotransfected成纤维细胞的处理而降低的胶质瘢痕形成。我们的研究结果表明,基于纳米转染的血管血管性细胞疗法(即非血管)细胞重编程代表了治疗缺血性卒中的有希望的策略。

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