Generation of Insulin-Expressing Cells in Mouse Small Intestine by Pdx1, MafA, and BETA2/NeuroD
BackgroundTo develop surrogate insulin-producing cells for diabetes therapy, adult stem cells have been identified in various tissues and studied for their conversion into β-cells. Pancreatic progenitor cells are derived from the endodermal epithelium and formed in a manner similar to gut progenitor...
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Korean Diabetes Association
2017-09-01
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doaj-4d55d193cd644d8ebae290bd82a5d9d62020-11-25T00:18:30ZengKorean Diabetes AssociationDiabetes & Metabolism Journal2233-60792233-60872017-09-0141540541610.4093/dmj.2017.41.5.405Generation of Insulin-Expressing Cells in Mouse Small Intestine by Pdx1, MafA, and BETA2/NeuroDSo-Hyun LeeMarie RheeJi-Won KimKun-Ho YoonBackgroundTo develop surrogate insulin-producing cells for diabetes therapy, adult stem cells have been identified in various tissues and studied for their conversion into β-cells. Pancreatic progenitor cells are derived from the endodermal epithelium and formed in a manner similar to gut progenitor cells. Here, we generated insulin-producing cells from the intestinal epithelial cells that induced many of the specific pancreatic transcription factors using adenoviral vectors carrying three genes: PMB (pancreatic and duodenal homeobox 1 [Pdx1], V-maf musculoaponeurotic fibrosarcoma oncogene homolog A [MafA], and BETA2/NeuroD).MethodsBy direct injection into the intestine through the cranial mesenteric artery, adenoviruses (Ad) were successfully delivered to the entire intestine. After virus injection, we could confirm that the small intestine of the mouse was appropriately infected with the Ad-Pdx1 and triple Ad-PMB.ResultsFour weeks after the injection, insulin mRNA was expressed in the small intestine, and the insulin gene expression was induced in Ad-Pdx1 and Ad-PMB compared to control Ad-green fluorescent protein. In addition, the conversion of intestinal cells into insulin-expressing cells was detected in parts of the crypts and villi located in the small intestine.ConclusionThese data indicated that PMB facilitate the differentiation of mouse intestinal cells into insulin-expressing cells. In conclusion, the small intestine is an accessible and abundant source of surrogate insulin-producing cells.https://e-dmj.org/Synapse/Data/PDFData/2004DMJ/dmj-41-405.pdfAdenoviridaeBeta cellsDifferentiationInjectionsIntestine, smallTranscription factors |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
So-Hyun Lee Marie Rhee Ji-Won Kim Kun-Ho Yoon |
spellingShingle |
So-Hyun Lee Marie Rhee Ji-Won Kim Kun-Ho Yoon Generation of Insulin-Expressing Cells in Mouse Small Intestine by Pdx1, MafA, and BETA2/NeuroD Diabetes & Metabolism Journal Adenoviridae Beta cells Differentiation Injections Intestine, small Transcription factors |
author_facet |
So-Hyun Lee Marie Rhee Ji-Won Kim Kun-Ho Yoon |
author_sort |
So-Hyun Lee |
title |
Generation of Insulin-Expressing Cells in Mouse Small Intestine by Pdx1, MafA, and BETA2/NeuroD |
title_short |
Generation of Insulin-Expressing Cells in Mouse Small Intestine by Pdx1, MafA, and BETA2/NeuroD |
title_full |
Generation of Insulin-Expressing Cells in Mouse Small Intestine by Pdx1, MafA, and BETA2/NeuroD |
title_fullStr |
Generation of Insulin-Expressing Cells in Mouse Small Intestine by Pdx1, MafA, and BETA2/NeuroD |
title_full_unstemmed |
Generation of Insulin-Expressing Cells in Mouse Small Intestine by Pdx1, MafA, and BETA2/NeuroD |
title_sort |
generation of insulin-expressing cells in mouse small intestine by pdx1, mafa, and beta2/neurod |
publisher |
Korean Diabetes Association |
series |
Diabetes & Metabolism Journal |
issn |
2233-6079 2233-6087 |
publishDate |
2017-09-01 |
description |
BackgroundTo develop surrogate insulin-producing cells for diabetes therapy, adult stem cells have been identified in various tissues and studied for their conversion into β-cells. Pancreatic progenitor cells are derived from the endodermal epithelium and formed in a manner similar to gut progenitor cells. Here, we generated insulin-producing cells from the intestinal epithelial cells that induced many of the specific pancreatic transcription factors using adenoviral vectors carrying three genes: PMB (pancreatic and duodenal homeobox 1 [Pdx1], V-maf musculoaponeurotic fibrosarcoma oncogene homolog A [MafA], and BETA2/NeuroD).MethodsBy direct injection into the intestine through the cranial mesenteric artery, adenoviruses (Ad) were successfully delivered to the entire intestine. After virus injection, we could confirm that the small intestine of the mouse was appropriately infected with the Ad-Pdx1 and triple Ad-PMB.ResultsFour weeks after the injection, insulin mRNA was expressed in the small intestine, and the insulin gene expression was induced in Ad-Pdx1 and Ad-PMB compared to control Ad-green fluorescent protein. In addition, the conversion of intestinal cells into insulin-expressing cells was detected in parts of the crypts and villi located in the small intestine.ConclusionThese data indicated that PMB facilitate the differentiation of mouse intestinal cells into insulin-expressing cells. In conclusion, the small intestine is an accessible and abundant source of surrogate insulin-producing cells. |
topic |
Adenoviridae Beta cells Differentiation Injections Intestine, small Transcription factors |
url |
https://e-dmj.org/Synapse/Data/PDFData/2004DMJ/dmj-41-405.pdf |
work_keys_str_mv |
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