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Citations to this article

iPSC-derived β cells model diabetes due to glucokinase deficiency
Haiqing Hua, … , Rudolph L. Leibel, Dieter Egli
Haiqing Hua, … , Rudolph L. Leibel, Dieter Egli
Published June 17, 2013
Citation Information: J Clin Invest. 2013;123(7):3146-3153. https://doi.org/10.1172/JCI67638.
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Technical Advance Article has an altmetric score of 64

iPSC-derived β cells model diabetes due to glucokinase deficiency

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Abstract

Diabetes is a disorder characterized by loss of β cell mass and/or β cell function, leading to deficiency of insulin relative to metabolic need. To determine whether stem cell–derived β cells recapitulate molecular-physiological phenotypes of a diabetic subject, we generated induced pluripotent stem cells (iPSCs) from subjects with maturity-onset diabetes of the young type 2 (MODY2), which is characterized by heterozygous loss of function of the gene encoding glucokinase (GCK). These stem cells differentiated into β cells with efficiency comparable to that of controls and expressed markers of mature β cells, including urocortin-3 and zinc transporter 8, upon transplantation into mice. While insulin secretion in response to arginine or other secretagogues was identical to that in cells from healthy controls, GCK mutant β cells required higher glucose levels to stimulate insulin secretion. Importantly, this glucose-specific phenotype was fully reverted upon gene sequence correction by homologous recombination. Our results demonstrate that iPSC-derived β cells reflect β cell–autonomous phenotypes of MODY2 subjects, providing a platform for mechanistic analysis of specific genotypes on β cell function.

Authors

Haiqing Hua, Linshan Shang, Hector Martinez, Matthew Freeby, Mary Pat Gallagher, Thomas Ludwig, Liyong Deng, Ellen Greenberg, Charles LeDuc, Wendy K. Chung, Robin Goland, Rudolph L. Leibel, Dieter Egli

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Total citations by year

Year: 2023 2021 2020 2019 2018 2017 2016 2015 2014 2013 2009 Total
Citations: 1 3 3 1 2 6 12 11 7 3 1 50
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Citations to this article (50)

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Diabetes 2023
Human Pluripotent Stem Cells Go Diabetic: A Glimpse on Monogenic Variants
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Frontiers in Endocrinology 2021
Current status and future prospects of patient-derived induced pluripotent stem cells
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Human Cell 2021
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2021
Gene-edited human stem cell–derived β cells from a patient with monogenic diabetes reverse preexisting diabetes in mice
KG Maxwell, P Augsornworawat, L Velazco-Cruz, MH Kim, R Asada, NJ Hogrebe, S Morikawa, F Urano, JR Millman
Science Translational Medicine 2020
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International journal of molecular sciences 2020
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L Velazco-Cruz, MM Goedegebuure, KG Maxwell, P Augsornworawat, NJ Hogrebe, JR Millman
Cell Reports 2020
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Circulation. Genomic and precision medicine 2018
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Scientific Reports 2017
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Arteriosclerosis, thrombosis, and vascular biology 2017
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Stem Cells Translational Medicine 2016
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Cell Stem Cell 2016
Report from IPITA-TTS Opinion Leaders Meeting on the Future of β-Cell Replacement:
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Nature Communications 2016
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Stem Cells International 2016
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Reversal of β cell de-differentiation by a small molecule inhibitor of the TGFβ pathway: ( A ) Immunostaining with antibodies against insulin (red) and Ucn3 (green) in pancreata from T2D (Lep Ob/Ob and Lepr Db/Db ), insulin-dependent diabetic (Ins2 Akita ), and healthy control (C57BL/6) mice. Ucn3 protein but not insulin protein is down regulated in diabetic pancreata compared to the healthy control. ( B ) Quantitative Real-Time PCR analysis of Ins1 and Ucn3 gene expression in islets from C57BL/6 ( n = 10), Lep Ob/Ob ( n = 9), Lepr Db/Db ( n = 8), and Ins2 Akita ( n = 11) mice. Ucn3 mRNA is significantly reduced in all diabetes models, while insulin mRNA is significantly reduced only in the most diabetic model (Ins2 Akita ). ( C ) Quantitative Real-Time PCR analysis of Ins1 and Ucn3 gene expression in islets from non-diabetic control mice ( n = 10; average blood glucose 167 ± 5 mg/dl), mildly diabetic ( n = 16; average blood glucose 381 ± 17 mg/dl) and severely diabetic mice ( n = 11; average blood glucose 588 ± 8 mg/dl). Error bars represent ±SEM. ***p < 0.001
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Cellular physiology and biochemistry : international journal of experimental cellular physiology, biochemistry, and pharmacology 2009

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