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In Vitro Differentiation of Human Umbilical Cord Blood CD133(+)Cells into Insulin Producing Cells in Co-Culture with Rat Pancreatic Mesenchymal Stem Cells

OBJECTIVE: Pancreatic stroma plays an important role in the induction of pancreatic cells by the use of close range signaling. In this respect, we presume that pancreatic mesenchymal cells (PMCs) as a fundamental factor of the stromal niche may have an effective role in differentiation of umbilical...

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Autores principales: Sahraneshin Samani, Fazel, Ebrahimi, Marzieh, Zandieh, Tahereh, Khoshchehreh, Reyhaneh, Baghaban Eslaminejad, Mohamadreza, Aghdami, Nasser, Baharvand, Hossein
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Royan Institute 2015
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Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4503835/
https://www.ncbi.nlm.nih.gov/pubmed/26199900
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author Sahraneshin Samani, Fazel
Ebrahimi, Marzieh
Zandieh, Tahereh
Khoshchehreh, Reyhaneh
Baghaban Eslaminejad, Mohamadreza
Aghdami, Nasser
Baharvand, Hossein
author_facet Sahraneshin Samani, Fazel
Ebrahimi, Marzieh
Zandieh, Tahereh
Khoshchehreh, Reyhaneh
Baghaban Eslaminejad, Mohamadreza
Aghdami, Nasser
Baharvand, Hossein
author_sort Sahraneshin Samani, Fazel
collection PubMed
description OBJECTIVE: Pancreatic stroma plays an important role in the induction of pancreatic cells by the use of close range signaling. In this respect, we presume that pancreatic mesenchymal cells (PMCs) as a fundamental factor of the stromal niche may have an effective role in differentiation of umbilical cord blood cluster of differentiation 133(+) (UCB-CD133(+)) cells into newly-formed β-cells in vitro. MATERIALS AND METHODS: This study is an experimental research. The UCB-CD133(+)cells were purified by magnetic activated cell sorting (MACS) and differentiated into insulin producing cells (IPCs) in co-culture, both directly and indirectly with rat PMCs. Immunocytochemistry and enzyme linked immune sorbent assay (ELISA) were used to determine expression and production of insulin and C-peptide at the protein level. RESULTS: Our results demonstrated that UCB-CD133(+)differentiated into IPCs. Cells in islet-like clusters with (out) co-cultured with rat pancreatic stromal cells produced insulin and C-peptide and released them into the culture medium at the end of the induction protocol. However they did not respond well to glucose challenges. CONCLUSION: Rat PMCs possibly affect differentiation of UCB-CD133(+)cells into IPCs by increasing the number of immature β-cells.
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spelling pubmed-45038352015-07-21 In Vitro Differentiation of Human Umbilical Cord Blood CD133(+)Cells into Insulin Producing Cells in Co-Culture with Rat Pancreatic Mesenchymal Stem Cells Sahraneshin Samani, Fazel Ebrahimi, Marzieh Zandieh, Tahereh Khoshchehreh, Reyhaneh Baghaban Eslaminejad, Mohamadreza Aghdami, Nasser Baharvand, Hossein Cell J Original Article OBJECTIVE: Pancreatic stroma plays an important role in the induction of pancreatic cells by the use of close range signaling. In this respect, we presume that pancreatic mesenchymal cells (PMCs) as a fundamental factor of the stromal niche may have an effective role in differentiation of umbilical cord blood cluster of differentiation 133(+) (UCB-CD133(+)) cells into newly-formed β-cells in vitro. MATERIALS AND METHODS: This study is an experimental research. The UCB-CD133(+)cells were purified by magnetic activated cell sorting (MACS) and differentiated into insulin producing cells (IPCs) in co-culture, both directly and indirectly with rat PMCs. Immunocytochemistry and enzyme linked immune sorbent assay (ELISA) were used to determine expression and production of insulin and C-peptide at the protein level. RESULTS: Our results demonstrated that UCB-CD133(+)differentiated into IPCs. Cells in islet-like clusters with (out) co-cultured with rat pancreatic stromal cells produced insulin and C-peptide and released them into the culture medium at the end of the induction protocol. However they did not respond well to glucose challenges. CONCLUSION: Rat PMCs possibly affect differentiation of UCB-CD133(+)cells into IPCs by increasing the number of immature β-cells. Royan Institute 2015 2015-07-11 /pmc/articles/PMC4503835/ /pubmed/26199900 Text en Any use, distribution, reproduction or abstract of this publication in any medium, with the exception of commercial purposes, is permitted provided the original work is properly cited http://creativecommons.org/licenses/by/2.5/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Article
Sahraneshin Samani, Fazel
Ebrahimi, Marzieh
Zandieh, Tahereh
Khoshchehreh, Reyhaneh
Baghaban Eslaminejad, Mohamadreza
Aghdami, Nasser
Baharvand, Hossein
In Vitro Differentiation of Human Umbilical Cord Blood CD133(+)Cells into Insulin Producing Cells in Co-Culture with Rat Pancreatic Mesenchymal Stem Cells
title In Vitro Differentiation of Human Umbilical Cord Blood CD133(+)Cells into Insulin Producing Cells in Co-Culture with Rat Pancreatic Mesenchymal Stem Cells
title_full In Vitro Differentiation of Human Umbilical Cord Blood CD133(+)Cells into Insulin Producing Cells in Co-Culture with Rat Pancreatic Mesenchymal Stem Cells
title_fullStr In Vitro Differentiation of Human Umbilical Cord Blood CD133(+)Cells into Insulin Producing Cells in Co-Culture with Rat Pancreatic Mesenchymal Stem Cells
title_full_unstemmed In Vitro Differentiation of Human Umbilical Cord Blood CD133(+)Cells into Insulin Producing Cells in Co-Culture with Rat Pancreatic Mesenchymal Stem Cells
title_short In Vitro Differentiation of Human Umbilical Cord Blood CD133(+)Cells into Insulin Producing Cells in Co-Culture with Rat Pancreatic Mesenchymal Stem Cells
title_sort in vitro differentiation of human umbilical cord blood cd133(+)cells into insulin producing cells in co-culture with rat pancreatic mesenchymal stem cells
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4503835/
https://www.ncbi.nlm.nih.gov/pubmed/26199900
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