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Development of a scalable method to isolate subsets of stem cell-derived pancreatic islet cells

Authors :
Audrey V. Parent
Sudipta Ashe
Gopika G. Nair
Mei-Lan Li
Jessica Chavez
Jennifer S. Liu
Yongping Zhong
Philip R. Streeter
Matthias Hebrok
Source :
Stem cell reports, vol 17, iss 4
Publication Year :
2022
Publisher :
eScholarship, University of California, 2022.

Abstract

Cell replacement therapy using β cells derived from stem cells is a promising alternative to conventional diabetes treatment options. Although current differentiation methods produce glucose-responsive β cells, they can also yield populations of undesired endocrine progenitors and other proliferating cell types that might interfere with long-term islet function and safety of transplanted cells. Here, we describe the generation of an array of monoclonal antibodies against cell surface markers that selectively label stem cell-derived islet cells. A high-throughput screen identified promising candidates, including three clones that mark a high proportion of endocrine cells in differentiated cultures. A scalable magnetic sorting method was developed to enrich for human pluripotent stem cell (hPSC)-derived islet cells using these three antibodies, leading to the formation of islet-like clusters with improved glucose-stimulated insulin secretion and reduced growth upon transplantation. This strategy should facilitate large-scale production of functional islet clusters from stem cells for disease modeling and cell replacement therapy.

Details

Database :
OpenAIRE
Journal :
Stem cell reports, vol 17, iss 4
Accession number :
edsair.doi.dedup.....94b5ca91d826ea7b59b75ce37c464716