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首页> 外文期刊>Biotechnology Progress >Proliferation and Differentiation of Mouse Embryonic Stem Cells in APA Microcapsule:A Model for Studying the Interaction between Stem Cells and Their Niche
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Proliferation and Differentiation of Mouse Embryonic Stem Cells in APA Microcapsule:A Model for Studying the Interaction between Stem Cells and Their Niche

机译:APA微胶囊中小鼠胚胎干细胞的增殖和分化:研究干细胞与其生态位相互作用的模型

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Embryonic stem (ES)cells hold promise either as an in vitro model recapitulating early embryonic development or as a renewable source of therapeutically useful cells.Certain aspects of the microenvironment (or niche)play critical roles in determining the fate of ES cells.Here,we reported the feasibility of using the technique of microencapsulation to study the interaction between ES cells and their tissue niche.ES cells'growth,viability,and differentiation in vitro were evaluated when they were enclosed in solid or liquefied core APA microcapsules.In comparison with those microcapsules with solid cores,the liquefied capsules provided a more suitable culture environment for the growth of ES cells.In addition,behavior of encapsulated ES cells in vivo was observed after their being implanted into mouse peritoneal cavities.In contrast to the prolonged lag phase in vitro,ES cells encapsulated grew much faster in vivo.Typical markers for the undifferentiated ES cells,such as AP,SSEA-1,and Oct-4 gene,were also tracked by immunochemistry and RT-PCR.Results showed that expression of markers remained high over 2 weeks of culture in vitro.However,decreased expression of markers was found in those samples in vivo with time passage.These findings implied that it was the combination of the intrinsic characteristics of ES cells and their microenvironment that regulated their fate.The APA-ES cells system may provide an optimal model to study the interaction between stem cells and their tissue niches.
机译:胚胎干细胞(ES)既可以作为概述早期胚胎发育的体外模型,又可以作为治疗有用细胞的可再生来源,因此具有广阔的前景。微环境(或利基)的某些方面在确定ES细胞的命运方面起着至关重要的作用。我们报道了使用微囊化技术研究ES细胞与其组织生态位之间相互作用的可行性。当将它们封装在固态或液化核心APA微胶囊中时,评估了ES细胞的生长,存活力和体外分化。这些具有固体核心的微胶囊,液化的胶囊为ES细胞的生长提供了更合适的培养环境。此外,在将封装的ES细胞植入小鼠腹膜腔后观察到其在体内的行为。在体外,被包封的ES细胞在体内生长得更快。未分化的ES细胞的典型标志物,如AP,SSEA-1和Oc还通过免疫化学和RT-PCR跟踪了t-4基因。结果显示,在体外培养2周内,标记物的表达仍然很高,但是随着时间的流逝,这些样品中的标记物表达降低了。这暗示着ES细胞的内在特性和它们的微环境的结合决定了它们的命运。APA-ES细胞系统可能为研究干细胞与其组织生态位之间的相互作用提供最佳模型。

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