首页> 外文期刊>Stem Cells >Bioluminescent imaging demonstrates that transplanted human embryonic stem cell-derived CD34(+) cells preferentially develop into endothelial cells.
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Bioluminescent imaging demonstrates that transplanted human embryonic stem cell-derived CD34(+) cells preferentially develop into endothelial cells.

机译:生物发光成像表明,移植的人类胚胎干细胞来源的CD34(+)细胞优先发展为内皮细胞。

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Human embryonic stem cells (hESCs) provide an important resource for novel regenerative medicine therapies and have been used to derive diverse cell populations, including hematopoietic and endothelial cells. However, it remains a challenge to achieve significant engraftment of hESC-derived blood cells when transplanted into animal models. To better understand mechanisms that enhance or limit the in vivo developmental potential of hESC-derived cells, we utilized hESCs that express firefly luciferase (luc) to allow noninvasive, real-time bioluminescent imaging of hESC-derived CD34(+) cells transplanted into the liver of neonatal immunodeficient mice. Serial imaging demonstrated stable engraftment and expansion of the luc(+) hESC-derived cells in vivo over several months. While we found that these hESC-derived CD34(+) cells have bipotential ability to generate both hematopoietic and endothelial lineages in vitro, these studies demonstrate preferential differentiation into endothelial cells in vivo, with only low levels of hematopoietic cell engraftment. Therefore, these studies reveal key differences in the developmental potential of hESC-derived cells using in vitro and in vivo analyses. Although transplanted hESC-derived CD34(+) cells are well-suited for revascularization therapies, additional measures are needed to provide higher levels of long-term hematopoietic engraftment.
机译:人类胚胎干细胞(hESCs)为新型再生医学疗法提供了重要资源,并已用于衍生多种细胞群体,包括造血和内皮细胞。然而,当移植到动物模型中时,实现hESC来源的血细胞的大量移植仍然是一个挑战。为了更好地了解增强或限制hESC来源的细胞在体内发育潜力的机制,我们利用表达萤火虫荧光素酶(luc)的hESC允许将hESC来源的CD34(+)细胞移植到小鼠体内进行非侵入性实时生物发光成像。新生儿免疫缺陷小鼠的肝脏。串行成像显示了几个月内体内稳定的luc(+)hESC衍生细胞的植入和扩增。虽然我们发现这些hESC衍生的CD34(+)细胞具有在体外产生造血和内皮细胞谱系的双能能力,但这些研究表明体内优先分化为内皮细胞,造血细胞植入水平较低。因此,这些研究使用体外和体内分析揭示了hESC衍生细胞发育潜力的关键差异。尽管移植的hESC来源的CD34(+)细胞非常适合进行血管重建治疗,但仍需要采取其他措施来提供更高水平的长期造血移植。

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