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117051 |
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|a dc
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|a Villani, Valentina
|e author
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|a Koch Institute for Integrative Cancer Research at MIT
|e contributor
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|a Cheng, Chia-Wei
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|a Yilmaz, Omer
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|a Buono, Roberta
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|a Wei, Min
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|a Kumar, Sanjeev
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|a Cohen, Pinchas
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|a Sneddon, Julie B.
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|a Perin, Laura
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|a Longo, Valter D.
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|a Cheng, Chia-Wei
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|a Yilmaz, Omer
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|a Fasting-Mimicking Diet Promotes Ngn3-Driven β-Cell Regeneration to Reverse Diabetes
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|b Elsevier BV,
|c 2018-07-23T18:50:49Z.
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|z Get fulltext
|u http://hdl.handle.net/1721.1/117051
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|a Stem-cell-based therapies can potentially reverse organ dysfunction and diseases, but the removal of impaired tissue and activation of a program leading to organ regeneration pose major challenges. In mice, a 4-day fasting mimicking diet (FMD) induces a stepwise expression of Sox17 and Pdx-1, followed by Ngn3-driven generation of insulin-producing β cells, resembling that observed during pancreatic development. FMD cycles restore insulin secretion and glucose homeostasis in both type 2 and type 1 diabetes mouse models. In human type 1 diabetes pancreatic islets, fasting conditions reduce PKA and mTOR activity and induce Sox2 and Ngn3 expression and insulin production. The effects of the FMD are reversed by IGF-1 treatment and recapitulated by PKA and mTOR inhibition. These results indicate that a FMD promotes the reprogramming of pancreatic cells to restore insulin generation in islets from T1D patients and reverse both T1D and T2D phenotypes in mouse models.
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|t Cell
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