Recapitulating endocrine cell clustering in culture promotes maturation of human stem-cell-derived β cells

Gopika G. Nair; Jennifer S. Liu; Holger A. Russ; Stella Tran; Michael S. Saxton; Richard Chen; Charity Juang; Mei lan Li; Vinh Q. Nguyen; Simone Giacometti; Sapna Puri; Yuan Xing; Yong Wang; Gregory L. Szot; Jose Oberholzer; Anil Bhushan; Matthias Hebrok

doi:10.1038/s41556-018-0271-4

Recapitulating endocrine cell clustering in culture promotes maturation of human stem-cell-derived β cells

Gopika G. Nair, Jennifer S. Liu, Holger A. Russ, Stella Tran, Michael S. Saxton, Richard Chen, Charity Juang, Mei lan Li, Vinh Q. Nguyen, Simone Giacometti, Sapna Puri, Yuan Xing, Yong Wang, Gregory L. Szot, Jose Oberholzer, Anil Bhushan, Matthias Hebrok

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Abstract

Despite advances in the differentiation of insulin-producing cells from human embryonic stem cells, the generation of mature functional β cells in vitro has remained elusive. To accomplish this goal, we have developed cell culture conditions to closely mimic events occurring during pancreatic islet organogenesis and β cell maturation. In particular, we have focused on recapitulating endocrine cell clustering by isolating and reaggregating immature β-like cells to form islet-sized enriched β-clusters (eBCs). eBCs display physiological properties analogous to primary human β cells, including robust dynamic insulin secretion, increased calcium signalling in response to secretagogues, and improved mitochondrial energization. Notably, endocrine cell clustering induces metabolic maturation by driving mitochondrial oxidative respiration, a process central to stimulus–secretion coupling in mature β cells. eBCs display glucose-stimulated insulin secretion as early as three days after transplantation in mice. In summary, replicating aspects of endocrine cell clustering permits the generation of stem-cell-derived β cells that resemble their endogenous counterparts.

Original language	English
Pages (from-to)	263-274
Number of pages	12
Journal	Nature Cell Biology
Volume	21
Issue number	2
DOIs	https://doi.org/10.1038/s41556-018-0271-4
State	Published - 1 Feb 2019
Externally published	Yes

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Nair, G. G., Liu, J. S., Russ, H. A., Tran, S., Saxton, M. S., Chen, R., Juang, C., Li, M. L., Nguyen, V. Q., Giacometti, S., Puri, S., Xing, Y., Wang, Y., Szot, G. L., Oberholzer, J., Bhushan, A., & Hebrok, M. (2019). Recapitulating endocrine cell clustering in culture promotes maturation of human stem-cell-derived β cells. Nature Cell Biology, 21(2), 263-274. https://doi.org/10.1038/s41556-018-0271-4

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title = "Recapitulating endocrine cell clustering in culture promotes maturation of human stem-cell-derived β cells",

abstract = "Despite advances in the differentiation of insulin-producing cells from human embryonic stem cells, the generation of mature functional β cells in vitro has remained elusive. To accomplish this goal, we have developed cell culture conditions to closely mimic events occurring during pancreatic islet organogenesis and β cell maturation. In particular, we have focused on recapitulating endocrine cell clustering by isolating and reaggregating immature β-like cells to form islet-sized enriched β-clusters (eBCs). eBCs display physiological properties analogous to primary human β cells, including robust dynamic insulin secretion, increased calcium signalling in response to secretagogues, and improved mitochondrial energization. Notably, endocrine cell clustering induces metabolic maturation by driving mitochondrial oxidative respiration, a process central to stimulus–secretion coupling in mature β cells. eBCs display glucose-stimulated insulin secretion as early as three days after transplantation in mice. In summary, replicating aspects of endocrine cell clustering permits the generation of stem-cell-derived β cells that resemble their endogenous counterparts.",

author = "Nair, {Gopika G.} and Liu, {Jennifer S.} and Russ, {Holger A.} and Stella Tran and Saxton, {Michael S.} and Richard Chen and Charity Juang and Li, {Mei lan} and Nguyen, {Vinh Q.} and Simone Giacometti and Sapna Puri and Yuan Xing and Yong Wang and Szot, {Gregory L.} and Jose Oberholzer and Anil Bhushan and Matthias Hebrok",

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year = "2019",

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Nair, GG, Liu, JS, Russ, HA, Tran, S, Saxton, MS, Chen, R, Juang, C, Li, ML, Nguyen, VQ, Giacometti, S, Puri, S, Xing, Y, Wang, Y, Szot, GL, Oberholzer, J, Bhushan, A & Hebrok, M 2019, 'Recapitulating endocrine cell clustering in culture promotes maturation of human stem-cell-derived β cells', Nature Cell Biology, vol. 21, no. 2, pp. 263-274. https://doi.org/10.1038/s41556-018-0271-4

TY - JOUR

T1 - Recapitulating endocrine cell clustering in culture promotes maturation of human stem-cell-derived β cells

AU - Nair, Gopika G.

AU - Liu, Jennifer S.

AU - Russ, Holger A.

AU - Tran, Stella

AU - Saxton, Michael S.

AU - Chen, Richard

AU - Juang, Charity

AU - Li, Mei lan

AU - Nguyen, Vinh Q.

AU - Giacometti, Simone

AU - Puri, Sapna

AU - Xing, Yuan

AU - Wang, Yong

AU - Szot, Gregory L.

AU - Oberholzer, Jose

AU - Bhushan, Anil

AU - Hebrok, Matthias

PY - 2019/2/1

Y1 - 2019/2/1

N2 - Despite advances in the differentiation of insulin-producing cells from human embryonic stem cells, the generation of mature functional β cells in vitro has remained elusive. To accomplish this goal, we have developed cell culture conditions to closely mimic events occurring during pancreatic islet organogenesis and β cell maturation. In particular, we have focused on recapitulating endocrine cell clustering by isolating and reaggregating immature β-like cells to form islet-sized enriched β-clusters (eBCs). eBCs display physiological properties analogous to primary human β cells, including robust dynamic insulin secretion, increased calcium signalling in response to secretagogues, and improved mitochondrial energization. Notably, endocrine cell clustering induces metabolic maturation by driving mitochondrial oxidative respiration, a process central to stimulus–secretion coupling in mature β cells. eBCs display glucose-stimulated insulin secretion as early as three days after transplantation in mice. In summary, replicating aspects of endocrine cell clustering permits the generation of stem-cell-derived β cells that resemble their endogenous counterparts.

AB - Despite advances in the differentiation of insulin-producing cells from human embryonic stem cells, the generation of mature functional β cells in vitro has remained elusive. To accomplish this goal, we have developed cell culture conditions to closely mimic events occurring during pancreatic islet organogenesis and β cell maturation. In particular, we have focused on recapitulating endocrine cell clustering by isolating and reaggregating immature β-like cells to form islet-sized enriched β-clusters (eBCs). eBCs display physiological properties analogous to primary human β cells, including robust dynamic insulin secretion, increased calcium signalling in response to secretagogues, and improved mitochondrial energization. Notably, endocrine cell clustering induces metabolic maturation by driving mitochondrial oxidative respiration, a process central to stimulus–secretion coupling in mature β cells. eBCs display glucose-stimulated insulin secretion as early as three days after transplantation in mice. In summary, replicating aspects of endocrine cell clustering permits the generation of stem-cell-derived β cells that resemble their endogenous counterparts.

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Recapitulating endocrine cell clustering in culture promotes maturation of human stem-cell-derived β cells

Abstract

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