Mitigating Ischemic Injury of Stem Cell-Derived Insulin-Producing Cells after Transplant

Gaetano Faleo; Holger A. Russ; Steven Wisel; Audrey V. Parent; Vinh Nguyen; Gopika G. Nair; Jonathan E. Freise; Karina E. Villanueva; Gregory L. Szot; Matthias Hebrok; Qizhi Tang

doi:10.1016/j.stemcr.2017.07.012

Mitigating Ischemic Injury of Stem Cell-Derived Insulin-Producing Cells after Transplant

Gaetano Faleo, Holger A. Russ, Steven Wisel, Audrey V. Parent, Vinh Nguyen, Gopika G. Nair, Jonathan E. Freise, Karina E. Villanueva, Gregory L. Szot, Matthias Hebrok, Qizhi Tang

Research output: Contribution to journal › Article › peer-review

43 Scopus citations

Abstract

The advent of large-scale in vitro differentiation of human stem cell-derived insulin-producing cells (SCIPC) has brought us closer to treating diabetes using stem cell technology. However, decades of experiences from islet transplantation show that ischemia-induced islet cell death after transplant severely limits the efficacy of the therapy. It is unclear to what extent human SCIPC are susceptible to ischemia. In this study, we show that more than half of SCIPC die shortly after transplantation. Nutrient deprivation and hypoxia acted synergistically to kill SCIPC in vitro. Amino acid supplementation rescued SCIPC from nutrient deprivation, likely by providing cellular energy. Generating SCIPC under physiological oxygen tension of 5% conferred hypoxia resistance without affecting their differentiation or function. A two-pronged strategy of physiological oxygen acclimatization during differentiation and amino acid supplementation during transplantation significantly improved SCIPC survival after transplant.

Original language	English
Pages (from-to)	807-819
Number of pages	13
Journal	Stem Cell Reports
Volume	9
Issue number	3
DOIs	https://doi.org/10.1016/j.stemcr.2017.07.012
State	Published - 12 Sep 2017
Externally published	Yes

Keywords

graft survival
hypoxia
ischemia
islet transplant
nutrient deprivation
stem cell-derived insulin-producing cells
type 1 diabetes

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1016/j.stemcr.2017.07.012

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title = "Mitigating Ischemic Injury of Stem Cell-Derived Insulin-Producing Cells after Transplant",

abstract = "The advent of large-scale in vitro differentiation of human stem cell-derived insulin-producing cells (SCIPC) has brought us closer to treating diabetes using stem cell technology. However, decades of experiences from islet transplantation show that ischemia-induced islet cell death after transplant severely limits the efficacy of the therapy. It is unclear to what extent human SCIPC are susceptible to ischemia. In this study, we show that more than half of SCIPC die shortly after transplantation. Nutrient deprivation and hypoxia acted synergistically to kill SCIPC in vitro. Amino acid supplementation rescued SCIPC from nutrient deprivation, likely by providing cellular energy. Generating SCIPC under physiological oxygen tension of 5% conferred hypoxia resistance without affecting their differentiation or function. A two-pronged strategy of physiological oxygen acclimatization during differentiation and amino acid supplementation during transplantation significantly improved SCIPC survival after transplant.",

keywords = "graft survival, hypoxia, ischemia, islet transplant, nutrient deprivation, stem cell-derived insulin-producing cells, type 1 diabetes",

author = "Gaetano Faleo and Russ, {Holger A.} and Steven Wisel and Parent, {Audrey V.} and Vinh Nguyen and Nair, {Gopika G.} and Freise, {Jonathan E.} and Villanueva, {Karina E.} and Szot, {Gregory L.} and Matthias Hebrok and Qizhi Tang",

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year = "2017",

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doi = "10.1016/j.stemcr.2017.07.012",

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AU - Faleo, Gaetano

AU - Russ, Holger A.

AU - Wisel, Steven

AU - Parent, Audrey V.

AU - Nguyen, Vinh

AU - Nair, Gopika G.

AU - Freise, Jonathan E.

AU - Villanueva, Karina E.

AU - Szot, Gregory L.

AU - Hebrok, Matthias

AU - Tang, Qizhi

PY - 2017/9/12

Y1 - 2017/9/12

N2 - The advent of large-scale in vitro differentiation of human stem cell-derived insulin-producing cells (SCIPC) has brought us closer to treating diabetes using stem cell technology. However, decades of experiences from islet transplantation show that ischemia-induced islet cell death after transplant severely limits the efficacy of the therapy. It is unclear to what extent human SCIPC are susceptible to ischemia. In this study, we show that more than half of SCIPC die shortly after transplantation. Nutrient deprivation and hypoxia acted synergistically to kill SCIPC in vitro. Amino acid supplementation rescued SCIPC from nutrient deprivation, likely by providing cellular energy. Generating SCIPC under physiological oxygen tension of 5% conferred hypoxia resistance without affecting their differentiation or function. A two-pronged strategy of physiological oxygen acclimatization during differentiation and amino acid supplementation during transplantation significantly improved SCIPC survival after transplant.

AB - The advent of large-scale in vitro differentiation of human stem cell-derived insulin-producing cells (SCIPC) has brought us closer to treating diabetes using stem cell technology. However, decades of experiences from islet transplantation show that ischemia-induced islet cell death after transplant severely limits the efficacy of the therapy. It is unclear to what extent human SCIPC are susceptible to ischemia. In this study, we show that more than half of SCIPC die shortly after transplantation. Nutrient deprivation and hypoxia acted synergistically to kill SCIPC in vitro. Amino acid supplementation rescued SCIPC from nutrient deprivation, likely by providing cellular energy. Generating SCIPC under physiological oxygen tension of 5% conferred hypoxia resistance without affecting their differentiation or function. A two-pronged strategy of physiological oxygen acclimatization during differentiation and amino acid supplementation during transplantation significantly improved SCIPC survival after transplant.

KW - graft survival

KW - hypoxia

KW - ischemia

KW - islet transplant

KW - nutrient deprivation

KW - stem cell-derived insulin-producing cells

KW - type 1 diabetes

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Mitigating Ischemic Injury of Stem Cell-Derived Insulin-Producing Cells after Transplant

Abstract

Keywords

UN SDGs

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