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Cell-Based Methods to Identify Inducers of Human Pancreatic Beta-Cell Proliferation.

Citation
Ackeifi, C. A., et al. “Cell-Based Methods To Identify Inducers Of Human Pancreatic Beta-Cell Proliferation.”. Methods In Molecular Biology (Clifton, N.j.), pp. 87-100.
Center Albert Einstein College of Medicine
Author Courtney A Ackeifi, Ethan A Swartz, Peng Wang
Keywords diabetes, Diabetes therapeutics, drug development, human islets, Human pancreatic beta cell, proliferation
Abstract

Diabetes is the result of the insufficiency or dysfunction of pancreatic beta cells alone or in combination with insulin resistance. The replacement or regeneration of beta cells can effectively reverse diabetes in humans and rodents. Therefore, the identification of novel small molecules that promote pancreatic beta-cell proliferation is an attractive approach for diabetic therapy. While numerous hormones, small molecules, and growth factors are able to drive rodent beta cells to replicate, only a few small molecules have demonstrated the ability to stimulate human beta-cell proliferation. Hence, there is an urgent need for therapeutic agents that induce regeneration and expansion of adult human beta cells. Here, we describe a detailed protocol for coating chamber slides, culturing primary islets, performing islet cell disassociation, seeding cells on chamber slides, treating islet cells with compounds or infecting them with adenovirus, immunostaining of proliferation markers and imaging, and data analysis.

Year of Publication
2018
Journal
Methods in molecular biology (Clifton, N.J.)
Volume
1787
Number of Pages
87-100
Date Published
12/2018
ISSN Number
1940-6029
DOI
10.1007/978-1-4939-7847-2_7
Alternate Journal
Methods Mol. Biol.
PMID
29736712
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