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A genetically engineered human pancreatic β cell line exhibiting glucose-inducible insulin secretion

机译:基因工程人胰岛β细胞系表现出葡萄糖诱导的胰岛素分泌

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摘要

Despite intense efforts over the past 30 years, human pancreatic β cell lines have not been available. Here, we describe a robust technology for producing a functional human β cell line using targeted oncogenesis in human fetal tissue. Human fetal pancreatic buds were transduced with a lentiviral vector that expressed SV40LT under the control of the insulin promoter. The transduced buds were then grafted into SCID mice so that they could develop into mature pancreatic tissue. Upon differentiation, the newly formed SV40LT-expressing β cells proliferated and formed insulinomas. The resulting β cells were then transduced with human telomerase reverse transcriptase (hTERT), grafted into other SCID mice, and finally expanded in vitro to generate cell lines. One of these cell lines, EndoC-βH1, expressed many β cell–specific markers without any substantial expression of markers of other pancreatic cell types. The cells secreted insulin when stimulated by glucose or other insulin secretagogues, and cell transplantation reversed chemically induced diabetes in mice. These cells represent a unique tool for large-scale drug discovery and provide a preclinical model for cell replacement therapy in diabetes. This technology could be generalized to generate other human cell lines when the cell type–specific promoter is available.
机译:尽管在过去30年中付出了巨大的努力,但人类胰腺β细胞系尚未获得。在这里,我们描述了一种在人的胎儿组织中使用靶向致癌作用生产功能性人β细胞系的可靠技术。用在胰岛素启动子控制下表达SV40LT的慢病毒载体转导人胎儿胰腺芽。然后将转导的芽移植到SCID小鼠中,使其可以发育成成熟的胰腺组织。通过分化,新形成的表达SV40LT的β细胞增殖并形成胰岛素瘤。然后用人端粒酶逆转录酶(hTERT)转导所得的β细胞,移植到其他SCID小鼠中,最后在体外扩增以生成细胞系。这些细胞系之一EndoC-βH1表达了许多β细胞特异性标记,而其他胰腺细胞类型的标记却没有任何实质性表达。当受到葡萄糖或其他胰岛素促分泌素刺激时,细胞会分泌胰岛素,而细胞移植可逆转小鼠化学诱导的糖尿病。这些细胞代表了大规模药物发现的独特工具,并为糖尿病中的细胞替代治疗提供了临床前模型。当特定于细胞类型的启动子可用时,可以将该技术普遍化以产生其他人类细胞系。

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