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Role of astroglia in Down’s syndrome revealed by patient-derived human-induced pluripotent stem cells

机译:由人源性人类多能干细胞揭示的星形胶质细胞在唐氏综合症中的作用

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Down’s syndrome (DS), caused by trisomy of human chromosome 21, is the most common genetic cause of intellectual disability. Here we use induced pluripotent stem cells (iPSCs) derived from DS patients to identify a role for astrocytes in DS pathogenesis. DS astroglia exhibit higher levels of reactive oxygen species and lower levels of synaptogenic molecules. Astrocyte-conditioned medium collected from DS astroglia causes toxicity to neurons, and fails to promote neuronal ion channel maturation and synapse formation. Transplantation studies show that DS astroglia do not promote neurogenesis of endogenous neural stem cells in vivo . We also observed abnormal gene expression profiles from DS astroglia. Finally, we show that the FDA-approved antibiotic drug, minocycline , partially corrects the pathological phenotypes of DS astroglia by specifically modulating the expression of S100B , GFAP , inducible nitric oxide synthase , and thrombospondins 1 and 2 in DS astroglia. Our studies shed light on the pathogenesis and possible treatment of DS by targeting astrocytes with a clinically available drug.
机译:由人类21号染色体三体性引起的唐氏综合症(DS)是智力残疾的最常见遗传原因。在这里,我们使用衍生自DS患者的诱导性多能干细胞(iPSC)来确定星形胶质细胞在DS发病机理中的作用。 DS星形胶质细胞具有较高水平的活性氧和较低水平的突触分子。从DS星形胶质细胞收集的星形胶质细胞条件培养基对神经元产生毒性,并且不能促进神经元离子通道的成熟和突触的形成。移植研究表明,DS星形胶质细胞不能促进体内内源性神经干细胞的神经发生。我们还观察到了来自DS星形胶质细胞的异常基因表达谱。最后,我们表明FDA批准的抗生素药物美满霉素可通过特异性调节DS星形胶质细胞中S100B,GFAP,诱导型一氧化氮合酶以及血小板反应蛋白1和2的表达来部分纠正DS星形胶质细胞的病理表型。我们的研究通过使用临床上可获得的药物靶向星形胶质细胞,揭示了DS的发病机理和可能的治疗方法。

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