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Do hematopoietic cells exposed to a neurogenic environment mimic properties of endogenous neural precursors?

机译:暴露于神经源性环境的造血细胞是否模仿内源性神经前体的特性?

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Hematopoietic progenitors are cells, which under challenging experimental conditions can develop unusual phenotypic properties, rather distant from their original mesodermal origin. As previously reported, cells derived from human umbilical cord blood (HUCB) or human bone marrow (BM) under certain in vivo or in vitro conditions can manifest neural features that resemble features of neural-derived cells, immunocytochemically and in some instances also morphologically. The present study explored how hematopoietic-derived cells would respond to neurogenic signals from the subventricular zone (SVZ) of adult and aged (6 and 16 months old) rats. The mononuclear fraction of HUCB cells was transplanted into the SVZ of immunosuppressed (single cyclosporin or three-drug treatment) animals. The triple-suppression paradigm allowed us to protect transplanted human cells within the brain and to explore further their phenotypic and migratory properties. One week after implantation, many surviving HUCB cells were located within the SVZ and the vertical limb of the rostral migratory stream (RMS). The migration of HUCB cells was restricted exclusively to the pathway leading to the olfactory bulb. In younger animals, grafted cells navigated almost halfway through the vertical limb, whereas, in the older animals, the migration was less pronounced. The overall cell survival was greater in younger animals than in older ones. Immunocytochemistry for surface CD antigen expression showed that many HUCB cells, either cultured or within the brain parenchyma, retained their hematopoietic identity. A few cells, identified by using human-specific antibodies (anti-human nuclei, or mitochondria) expressed nestin and doublecortin, markers of endogenous neural progenitors. Therefore, it is believed that the environment of the neurogenic SVZ, even in aged animals, was able to support survival, "neuralization," and migratory features of HUCB-derived cells.
机译:造血祖细胞是细胞,在具有挑战性的实验条件下,它们可能会发育出异常的表型特性,与原始的中胚层起源相去甚远。如先前报道的,在某些体内或体外条件下,源自人脐带血(HUCB)或人骨髓(BM)的细胞在免疫细胞化学上以及在某些情况下在形态上也可表现出类似于神经源细胞特征的神经特征。本研究探讨了造血细胞如何对成年和成年(6和16个月大)大鼠脑室下区域(SVZ)的神经源信号作出反应。将HUCB细胞的单核部分移植到免疫抑制的动物(单环孢菌素或三药治疗)的SVZ中。三重抑制范例使我们能够保护大脑中移植的人类细胞,并进一步探索其表型和迁移特性。植入后一周,许多幸存的HUCB细胞位于SVZ内和延髓游流(RMS)的垂直肢体中。 HUCB细胞的迁移只限于导致嗅球的途径。在较年轻的动物中,嫁接的细胞几乎穿过垂直肢体的一半,而在较年长的动物中,迁移不太明显。幼小动物的总细胞存活率要大于大龄动物。用于表面CD抗原表达的免疫细胞化学显示,许多HUCB细胞(无论是培养的还是脑实质内的细胞)都保留了其造血特性。通过使用人类特异性抗体(抗人类核或线粒体)鉴定出的一些细胞表达了Nestin和Doublecortin(内源性神经祖细胞的标志物)。因此,可以相信,即使在老年动物中,神经源性SVZ的环境也能够支持HUCB衍生细胞的存活,“神经化”和迁移特征。

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