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Transcription Factors in Pancreatic Dewelopment Animal Models

机译:胰腺发育式动物模型中的转录因子

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Through the analysis of genetically modified mice a hierarchy of transcription factors regulating pancreas specification, endocrine destiny as well as endocrine subtype specification and differentiation has been established. In addition to conventional approaches such as transgenic technologies and gene targeting, recombinase fate mapping in mice has been key in establishing the lineage relationship between progenitor cells and their progeny in understanding pancreas formation. Moreover, the design of specific mouse models to conditionally express transcription factors in different populations of progenitor cells has revealed to what extent transcription factors required for islet cell development are also sufficient to induce endocrine differentiation and the importance of the competence of progenitor cells to respond to the genetic program implemented by these factors. Taking advantage of this basic science knowledge acquired in rodents, immature insulin-producing cells have recently been differentiated in vitro from human embryonic stem cells. Taken together these major advances emphasize the need to gain further in-depth knowledge of the molecular and cellular mechanisms controlling beta-celI differentiation in mice to generate functional beta-cells in the future that could be used for cell therapy in diabetes.
机译:通过分析转基因的转录因子等级调节胰腺规范,内分泌命运以及内分泌亚型规范和分化。除了常规的方法在建立祖细胞和它们在理解胰腺形成子代之间的关系谱系如转基因技术和基因定位,在小鼠中的重组酶命运映射一直键。此外,特定的小鼠模型中祖细胞的不同人群条件性表达转录因子的设计已经透露给什么需要胰岛细胞的发育程度转录因子也足以引起内分泌分化细胞和祖细胞的能力以应对重要性由这些因素实施的遗传计划。利用在啮齿动物中获得的这种基本的科学知识,最近在人胚胎干细胞体外分化了不成熟的胰岛素产生细胞。这些主要进步强调,需要进一步深入了解控制小鼠的ββ细胞分化的分子和细胞机制,以便在未来产生功能β细胞,可用于糖尿病中的细胞疗法。

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