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Revealing transcription factors during human pancreatic β cell development

机译:在人类胰腺β细胞发育过程中揭示转录因子

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Developing cell-based diabetes therapies requires examining transcriptional mechanisms underlying human β cell development. However, increased knowledge is hampered by low availability of fetal pancreatic tissue and gene targeting strategies. Rodent models have elucidated transcription factor roles during islet organogenesis and maturation, but differences between mouse and human islets have been identified. The past 5 years have seen strides toward generating human β cell lines, the examination of human transcription factor expression, and studies utilizing induced pluripotent stem cells (iPS cells) and human embryonic stem (hES) cells to generate β-like cells. Nevertheless, much remains to be resolved. We present current knowledge of developing human β cell transcription factor expression, as compared to rodents. We also discuss recent studies employing transcription factor or epigenetic modulation to generate β cells.
机译:发展基于细胞的糖尿病疗法需要检查人类β细胞发育的转录机制。然而,胎儿胰腺组织的低可用性和基因靶向策略阻碍了知识的增长。啮齿动物模型已经阐明了胰岛器官发生和成熟过程中转录因子的作用,但是已经确定了小鼠和人类胰岛之间的差异。在过去的5年中,在生成人β细胞系,检查人类转录因子表达以及利用诱导性多能干细胞(iPS细胞)和人胚胎干(hES)细胞生成β样细胞方面取得了长足进步。尽管如此,仍有许多问题有待解决。我们提供与啮齿类动物相比发展人类β细胞转录因子表达的当前知识。我们还将讨论利用转录因子或表观遗传调制产生β细胞的最新研究。

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