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脑缺血后血管周细胞具有多能干细胞活性,可分化为神经和血管谱系细胞。

Brain vascular pericytes following ischemia have multipotential stem cell activity to differentiate into neural and vascular lineage cells.

机构信息

Institute for Advanced Medical Sciences, Nishinomiya, Hyogo, Japan.

Department of Genetics, Hyogo College of Medicine, Nishinomiya, Hyogo, Japan.

出版信息

Stem Cells. 2015 Jun;33(6):1962-74. doi: 10.1002/stem.1977. Epub 2015 Apr 23.

Abstract

Brain vascular pericytes (PCs) are a key component of the blood-brain barrier (BBB)/neurovascular unit, along with neural and endothelial cells. Besides their crucial role in maintaining the BBB, increasing evidence shows that PCs have multipotential stem cell activity. However, their multipotency has not been considered in the pathological brain, such as after an ischemic stroke. Here, we examined whether brain vascular PCs following ischemia (iPCs) have multipotential stem cell activity and differentiate into neural and vascular lineage cells to reconstruct the BBB/neurovascular unit. Using PCs extracted from ischemic regions (iPCs) from mouse brains and human brain PCs cultured under oxygen/glucose deprivation, we show that PCs developed stemness presumably through reprogramming. The iPCs revealed a complex phenotype of angioblasts, in addition to their original mesenchymal properties, and multidifferentiated into cells from both a neural and vascular lineage. These data indicate that under ischemic/hypoxic conditions, PCs can acquire multipotential stem cell activity and can differentiate into major components of the BBB/neurovascular unit. Thus, these findings support the novel concept that iPCs can contribute to both neurogenesis and vasculogenesis at the site of brain injuries.

摘要

脑血管周细胞(PCs)是血脑屏障(BBB)/神经血管单元的重要组成部分,与神经细胞和内皮细胞一起。除了在维持 BBB 方面的关键作用外,越来越多的证据表明 PCs 具有多能干细胞活性。然而,它们的多能性在病理性大脑中并未被考虑,例如在缺血性中风后。在这里,我们研究了缺血后的脑血管 PCs(iPCs)是否具有多能干细胞活性,并分化为神经和血管谱系细胞来重建 BBB/神经血管单元。使用从缺血区域提取的 PC(iPCs)和在缺氧/葡萄糖剥夺条件下培养的人脑 PC,我们表明 PC 通过重编程获得了干细胞特性。iPCs 除了具有原始的间充质特性外,还表现出了成血管细胞的复杂表型,并多能性分化为神经和血管谱系的细胞。这些数据表明,在缺血/缺氧条件下,PCs 可以获得多能干细胞活性,并分化为 BBB/神经血管单元的主要组成部分。因此,这些发现支持了一个新的概念,即 iPCs 可以在脑损伤部位促进神经发生和血管生成。

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