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

Research output: Contribution to journalArticlepeer-review

383 Scopus citations

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 languageEnglish
Pages (from-to)263-274
Number of pages12
JournalNature Cell Biology
Volume21
Issue number2
DOIs
StatePublished - 1 Feb 2019
Externally publishedYes

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