In vitro quantitative and relative gene expression analysis of pancreatic transcription factors Pdx‐1, Ngn‐3, Isl‐1, Pax‐4, Pax‐6 and Nkx‐6.1 in trans‐differentiated human hepatic progenitors

AIMS/INTRODUCTION: Diabetes is a major health concern throughout the world because of its increasing prevalence in epidemic proportions. β‐Cell deterioration in the pancreas is a crucial factor for the progression of diabetes mellitus. Therefore, the restoration of β‐cell mass and its function is of...

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Autores principales: Vishwakarma, Sandeep Kumar, Rahamathulla, Syed, Bardia, Avinash, Tiwari, Santosh K, Srinivas, Gunda, Raj, Avinash, Tripura, Chaturvedula, Sandhya, Annamaneni, Habeeb, Mohammed Aejaz, Khan, Aleem A, Pande, Gopal, Reddy, K Pratap, Reddy, P Yugandhar
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Wiley-Blackwell 2014
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Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4188105/
https://www.ncbi.nlm.nih.gov/pubmed/25411615
http://dx.doi.org/10.1111/jdi.12193
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author Vishwakarma, Sandeep Kumar
Rahamathulla, Syed
Bardia, Avinash
Tiwari, Santosh K
Srinivas, Gunda
Raj, Avinash
Tripura, Chaturvedula
Sandhya, Annamaneni
Habeeb, Mohammed Aejaz
Khan, Aleem A
Pande, Gopal
Reddy, K Pratap
Reddy, P Yugandhar
author_facet Vishwakarma, Sandeep Kumar
Rahamathulla, Syed
Bardia, Avinash
Tiwari, Santosh K
Srinivas, Gunda
Raj, Avinash
Tripura, Chaturvedula
Sandhya, Annamaneni
Habeeb, Mohammed Aejaz
Khan, Aleem A
Pande, Gopal
Reddy, K Pratap
Reddy, P Yugandhar
author_sort Vishwakarma, Sandeep Kumar
collection PubMed
description AIMS/INTRODUCTION: Diabetes is a major health concern throughout the world because of its increasing prevalence in epidemic proportions. β‐Cell deterioration in the pancreas is a crucial factor for the progression of diabetes mellitus. Therefore, the restoration of β‐cell mass and its function is of vital importance for the development of effective therapeutic strategies and most accessible cell sources for the treatment of diabetes mellitus. MATERIALS AND METHODS: Human fetuses (12–20 weeks gestation age) were used to isolate human hepatic progenitor cells (hHPCs) from fetal liver using a two‐step collagenase digestion method. Epithelial cell adhesion molecule‐positive (EpCAM+ve)‐enriched hHPCs were cultured in vitro and induced with 5–30 mmol/L concentration of glucose for 0–32 h. Pdx‐1 expression and insulin secretion was analyzed using immunophenotypic and chemifluorescence assays, respectively. Relative gene expression was quantified in induced hHPCs, and compared with uninduced and pancreatic cells to identify the activated transcription factors (Pdx‐1, Ngn‐3, Isl‐1, Pax‐4, Pax‐6 and Nkx‐6.1) involved in β‐cell production. RESULTS: EpCAM+ve cells derived from human fetal liver showed high in vitro trans‐differentiation potential towards the β‐cell phenotype with 23 mmol/L glucose induction after 24 h. The transcription factors showed eminent expression in induced cells. The expression level of transcription factors was found significantly high in 23 mmol/L‐induced hHPCs as compared with the uninduced cells. CONCLUSIONS: The present study has shown an exciting new insight into β‐cell development from hHPCs trans‐differentiation. Relative quantification of gene expression in trans‐differentiated cells offers vast possibility for the production of a maximum number of functionally active pancreatic β‐cells for a future cure of diabetes.
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spelling pubmed-41881052014-11-19 In vitro quantitative and relative gene expression analysis of pancreatic transcription factors Pdx‐1, Ngn‐3, Isl‐1, Pax‐4, Pax‐6 and Nkx‐6.1 in trans‐differentiated human hepatic progenitors Vishwakarma, Sandeep Kumar Rahamathulla, Syed Bardia, Avinash Tiwari, Santosh K Srinivas, Gunda Raj, Avinash Tripura, Chaturvedula Sandhya, Annamaneni Habeeb, Mohammed Aejaz Khan, Aleem A Pande, Gopal Reddy, K Pratap Reddy, P Yugandhar J Diabetes Investig Articles AIMS/INTRODUCTION: Diabetes is a major health concern throughout the world because of its increasing prevalence in epidemic proportions. β‐Cell deterioration in the pancreas is a crucial factor for the progression of diabetes mellitus. Therefore, the restoration of β‐cell mass and its function is of vital importance for the development of effective therapeutic strategies and most accessible cell sources for the treatment of diabetes mellitus. MATERIALS AND METHODS: Human fetuses (12–20 weeks gestation age) were used to isolate human hepatic progenitor cells (hHPCs) from fetal liver using a two‐step collagenase digestion method. Epithelial cell adhesion molecule‐positive (EpCAM+ve)‐enriched hHPCs were cultured in vitro and induced with 5–30 mmol/L concentration of glucose for 0–32 h. Pdx‐1 expression and insulin secretion was analyzed using immunophenotypic and chemifluorescence assays, respectively. Relative gene expression was quantified in induced hHPCs, and compared with uninduced and pancreatic cells to identify the activated transcription factors (Pdx‐1, Ngn‐3, Isl‐1, Pax‐4, Pax‐6 and Nkx‐6.1) involved in β‐cell production. RESULTS: EpCAM+ve cells derived from human fetal liver showed high in vitro trans‐differentiation potential towards the β‐cell phenotype with 23 mmol/L glucose induction after 24 h. The transcription factors showed eminent expression in induced cells. The expression level of transcription factors was found significantly high in 23 mmol/L‐induced hHPCs as compared with the uninduced cells. CONCLUSIONS: The present study has shown an exciting new insight into β‐cell development from hHPCs trans‐differentiation. Relative quantification of gene expression in trans‐differentiated cells offers vast possibility for the production of a maximum number of functionally active pancreatic β‐cells for a future cure of diabetes. Wiley-Blackwell 2014-01-29 2014-09 /pmc/articles/PMC4188105/ /pubmed/25411615 http://dx.doi.org/10.1111/jdi.12193 Text en © 2014 The Authors. Journal of Diabetes Investigation published by Asian Association for the Study of Diabetes (AASD) and Wiley Publishing Asia Pty Ltd This is an open access article under the terms of the Creative Commons Attribution‐NonCommercial‐NoDerivs (http://creativecommons.org/licenses/by-nc-nd/3.0/) License, which permits use and distribution in any medium, provided the original work is properly cited, the use is non‐commercial and no modifications or adaptations are made.
spellingShingle Articles
Vishwakarma, Sandeep Kumar
Rahamathulla, Syed
Bardia, Avinash
Tiwari, Santosh K
Srinivas, Gunda
Raj, Avinash
Tripura, Chaturvedula
Sandhya, Annamaneni
Habeeb, Mohammed Aejaz
Khan, Aleem A
Pande, Gopal
Reddy, K Pratap
Reddy, P Yugandhar
In vitro quantitative and relative gene expression analysis of pancreatic transcription factors Pdx‐1, Ngn‐3, Isl‐1, Pax‐4, Pax‐6 and Nkx‐6.1 in trans‐differentiated human hepatic progenitors
title In vitro quantitative and relative gene expression analysis of pancreatic transcription factors Pdx‐1, Ngn‐3, Isl‐1, Pax‐4, Pax‐6 and Nkx‐6.1 in trans‐differentiated human hepatic progenitors
title_full In vitro quantitative and relative gene expression analysis of pancreatic transcription factors Pdx‐1, Ngn‐3, Isl‐1, Pax‐4, Pax‐6 and Nkx‐6.1 in trans‐differentiated human hepatic progenitors
title_fullStr In vitro quantitative and relative gene expression analysis of pancreatic transcription factors Pdx‐1, Ngn‐3, Isl‐1, Pax‐4, Pax‐6 and Nkx‐6.1 in trans‐differentiated human hepatic progenitors
title_full_unstemmed In vitro quantitative and relative gene expression analysis of pancreatic transcription factors Pdx‐1, Ngn‐3, Isl‐1, Pax‐4, Pax‐6 and Nkx‐6.1 in trans‐differentiated human hepatic progenitors
title_short In vitro quantitative and relative gene expression analysis of pancreatic transcription factors Pdx‐1, Ngn‐3, Isl‐1, Pax‐4, Pax‐6 and Nkx‐6.1 in trans‐differentiated human hepatic progenitors
title_sort in vitro quantitative and relative gene expression analysis of pancreatic transcription factors pdx‐1, ngn‐3, isl‐1, pax‐4, pax‐6 and nkx‐6.1 in trans‐differentiated human hepatic progenitors
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4188105/
https://www.ncbi.nlm.nih.gov/pubmed/25411615
http://dx.doi.org/10.1111/jdi.12193
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