PAX4 enhances beta-cell differentiation of human embryonic stem cells.

BACKGROUND:Human embryonic stem cells (HESC) readily differentiate into an apparently haphazard array of cell types, corresponding to all three germ layers, when their culture conditions are altered, for example by growth in suspension as aggregates known as embryoid bodies (EBs). However, this dive...

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Main Authors: Chee Gee Liew, Nadia N Shah, Sarah J Briston, Ruth M Shepherd, Cheen Peen Khoo, Mark J Dunne, Harry D Moore, Karen E Cosgrove, Peter W Andrews
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2008-03-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC2262135?pdf=render
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spelling doaj-c797fd1a21b54eddb11c832de0f192032020-11-25T01:21:29ZengPublic Library of Science (PLoS)PLoS ONE1932-62032008-03-0133e178310.1371/journal.pone.0001783PAX4 enhances beta-cell differentiation of human embryonic stem cells.Chee Gee LiewNadia N ShahSarah J BristonRuth M ShepherdCheen Peen KhooMark J DunneHarry D MooreKaren E CosgrovePeter W AndrewsBACKGROUND:Human embryonic stem cells (HESC) readily differentiate into an apparently haphazard array of cell types, corresponding to all three germ layers, when their culture conditions are altered, for example by growth in suspension as aggregates known as embryoid bodies (EBs). However, this diversity of differentiation means that the efficiency of producing any one particular cell type is inevitably low. Although pancreatic differentiation has been reported from HESC, practicable applications for the use of beta-cells derived from HESC to treat diabetes will only be possible once techniques are developed to promote efficient differentiation along the pancreatic lineages. METHODS AND FINDINGS:Here, we have tested whether the transcription factor, Pax4 can be used to drive the differentiation of HESC to a beta-cell fate in vitro. We constitutively over-expressed Pax4 in HESCs by stable transfection, and used Q-PCR analysis, immunocytochemistry, ELISA, Ca(2+) microfluorimetry and cell imaging to assess the role of Pax4 in the differentiation and intracellular Ca(2+) homeostasis of beta-cells developing in embryoid bodies produced from such HESC. Cells expressing key beta-cell markers were isolated by fluorescence-activated cell sorting after staining for high zinc content using the vital dye, Newport Green. CONCLUSION:Constitutive expression of Pax4 in HESC substantially enhances their propensity to form putative beta-cells. Our findings provide a novel foundation to study the mechanism of pancreatic beta-cells differentiation during early human development and to help evaluate strategies for the generation of purified beta-cells for future clinical applications.http://europepmc.org/articles/PMC2262135?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Chee Gee Liew
Nadia N Shah
Sarah J Briston
Ruth M Shepherd
Cheen Peen Khoo
Mark J Dunne
Harry D Moore
Karen E Cosgrove
Peter W Andrews
spellingShingle Chee Gee Liew
Nadia N Shah
Sarah J Briston
Ruth M Shepherd
Cheen Peen Khoo
Mark J Dunne
Harry D Moore
Karen E Cosgrove
Peter W Andrews
PAX4 enhances beta-cell differentiation of human embryonic stem cells.
PLoS ONE
author_facet Chee Gee Liew
Nadia N Shah
Sarah J Briston
Ruth M Shepherd
Cheen Peen Khoo
Mark J Dunne
Harry D Moore
Karen E Cosgrove
Peter W Andrews
author_sort Chee Gee Liew
title PAX4 enhances beta-cell differentiation of human embryonic stem cells.
title_short PAX4 enhances beta-cell differentiation of human embryonic stem cells.
title_full PAX4 enhances beta-cell differentiation of human embryonic stem cells.
title_fullStr PAX4 enhances beta-cell differentiation of human embryonic stem cells.
title_full_unstemmed PAX4 enhances beta-cell differentiation of human embryonic stem cells.
title_sort pax4 enhances beta-cell differentiation of human embryonic stem cells.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2008-03-01
description BACKGROUND:Human embryonic stem cells (HESC) readily differentiate into an apparently haphazard array of cell types, corresponding to all three germ layers, when their culture conditions are altered, for example by growth in suspension as aggregates known as embryoid bodies (EBs). However, this diversity of differentiation means that the efficiency of producing any one particular cell type is inevitably low. Although pancreatic differentiation has been reported from HESC, practicable applications for the use of beta-cells derived from HESC to treat diabetes will only be possible once techniques are developed to promote efficient differentiation along the pancreatic lineages. METHODS AND FINDINGS:Here, we have tested whether the transcription factor, Pax4 can be used to drive the differentiation of HESC to a beta-cell fate in vitro. We constitutively over-expressed Pax4 in HESCs by stable transfection, and used Q-PCR analysis, immunocytochemistry, ELISA, Ca(2+) microfluorimetry and cell imaging to assess the role of Pax4 in the differentiation and intracellular Ca(2+) homeostasis of beta-cells developing in embryoid bodies produced from such HESC. Cells expressing key beta-cell markers were isolated by fluorescence-activated cell sorting after staining for high zinc content using the vital dye, Newport Green. CONCLUSION:Constitutive expression of Pax4 in HESC substantially enhances their propensity to form putative beta-cells. Our findings provide a novel foundation to study the mechanism of pancreatic beta-cells differentiation during early human development and to help evaluate strategies for the generation of purified beta-cells for future clinical applications.
url http://europepmc.org/articles/PMC2262135?pdf=render
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