首页> 外文期刊>Immunology: An Official Journal of the British Society for Immunology >Intranasal delivery of central nervous system-retargeted human mesenchymal stromal cells prolongs treatment efficacy of experimental autoimmune encephalomyelitis
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Intranasal delivery of central nervous system-retargeted human mesenchymal stromal cells prolongs treatment efficacy of experimental autoimmune encephalomyelitis

机译:经鼻中枢神经系统靶向的人间充质基质细胞的鼻内递送延长了实验性自身免疫性脑脊髓炎的治疗效果

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Summary: Treatment with mesenchymal stromal cells (MSCs) is currently of interest for a number of diseases including multiple sclerosis. MSCs are known to target inflamed tissues, but in a therapeutic setting their systemic administration will lead to few cells reaching the brain. We hypothesized that MSCs may target the brain upon intranasal administration and persist in central nervous system (CNS) tissue if expressing a CNS-targeting receptor. To demonstrate proof of concept, MSCs were genetically engineered to express a myelin oligodendrocyte glycoprotein-specific receptor. Engineered MSCs retained their immunosuppressive capacity, infiltrated into the brain upon intranasal cell administration, and were able to significantly reduce disease symptoms of experimental autoimmune encephalomyelitis (EAE). Mice treated with CNS-targeting MSCs were resistant to further EAE induction whereas non-targeted MSCs did not give such persistent effects. Histological analysis revealed increased brain restoration in engineered MSC-treated mice. In conclusion, MSCs can be genetically engineered to target the brain and prolong therapeutic efficacy in an EAE model.
机译:简介:对于许多疾病,包括多发性硬化症,间充质基质细胞(MSC)治疗目前是令人关注的。已知MSC靶向发炎的组织,但在治疗环境中,它们的全身性给药将导致很少的细胞到达大脑。我们假设,MSCs经鼻内给药后可能靶向大脑,并且如果表达靶向CNS的受体,则可以持续存在于中枢神经系统(CNS)组织中。为了证明概念证明,对MSC进行了基因工程改造以表达髓磷脂少突胶质细胞糖蛋白特异性受体。经过改造的MSC保留了其免疫抑制能力,在鼻内给药后渗透到大脑中,并且能够显着减轻实验性自身免疫性脑脊髓炎(EAE)的疾病症状。用靶向CNS的MSC治疗的小鼠对进一步的EAE诱导具有抗性,而未靶向的MSC则没有这种持久的作用。组织学分析显示,经工程改造的MSC处理的小鼠的大脑恢复增强。总之,可以对MSCs进行基因工程改造,使其靶向大脑并延长EAE模型中的治疗效果。

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