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Pancreatic Pseudoislets: An Organoid Archetype for Metabolism Research.

Citation
Friedlander, M. S. H., et al. “Pancreatic Pseudoislets: An Organoid Archetype For Metabolism Research.”. Diabetes, pp. 1051-1060.
Center Stanford University
Author Mollie S H Friedlander, Vy M Nguyen, Seung K Kim, Romina J Bevacqua
Abstract

Pancreatic islets are vital endocrine regulators of systemic metabolism, and recent investigations have increasingly focused on understanding human islet biology. Studies of isolated human islets have advanced understanding of the development, function, and regulation of cells comprising islets, especially pancreatic - and -cells. However, the multicellularity of the intact islet has stymied specific experimental approaches-particularly in genetics and cell signaling interrogation. This barrier has been circumvented by the observation that islet cells can survive dispersion and reaggregate to form "pseudoislets," organoids that retain crucial physiological functions, including regulated insulin and glucagon secretion. Recently, exciting advances in the use of pseudoislets for genetics, genomics, islet cell transplantation, and studies of intraislet signaling and islet cell interactions have been reported by investigators worldwide. Here we review molecular and cellular mechanisms thought to promote islet cell reaggregation, summarize methods that optimize pseudoislet development, and detail recent insights about human islet biology from genetic and transplantation-based pseudoislet experiments. Owing to robust, international programs for procuring primary human pancreata, pseudoislets should serve as both a durable paradigm for primary organoid studies and as an engine of discovery for islet biology, diabetes, and metabolism research.

Year of Publication
2021
Journal
Diabetes
Volume
70
Issue
5
Number of Pages
1051-1060
Date Published
12/2021
ISSN Number
1939-327X
DOI
10.2337/db20-1115
Alternate Journal
Diabetes
PMID
33947722
PMCID
PMC8343609
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