FOXO1 inhibition yields functional insulin-producing cells in human gut organoid cultures

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作者
Ryotaro Bouchi
Kylie S. Foo
Haiqing Hua
Kyoichiro Tsuchiya
Yoshiaki Ohmura
P. Rodrigo Sandoval
Lloyd E. Ratner
Dieter Egli
Rudolph L. Leibel
Domenico Accili
机构
[1] Columbia University College of Physicians and Surgeons,Department of Medicine
[2] New York Stem Cell Foundation Research Institute,Department of Pediatrics
[3] Columbia University College of Physicians and Surgeons,Department of Surgery
[4] Tokyo Medical and Dental University,undefined
[5] Columbia University College of Physicians and Surgeons,undefined
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Generation of surrogate sources of insulin-producing β-cells remains a goal of diabetes therapy. While most efforts have been directed at differentiating embryonic or induced pluripotent stem (iPS) cells into β-like-cells through endodermal progenitors, we have shown that gut endocrine progenitor cells of mice can be differentiated into glucose-responsive, insulin-producing cells by ablation of transcription factor Foxo1. Here we show that FOXO1 is present in human gut endocrine progenitor and serotonin-producing cells. Using gut organoids derived from human iPS cells, we show that FOXO1 inhibition using a dominant-negative mutant or lentivirus-encoded small hairpin RNA promotes generation of insulin-positive cells that express all markers of mature pancreatic β-cells, release C-peptide in response to secretagogues and survive in vivo following transplantation into mice. The findings raise the possibility of using gut-targeted FOXO1 inhibition or gut organoids as a source of insulin-producing cells to treat human diabetes.
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