Diabetes and tumor formation in transgenic mice expressing Reg I

Takashi Yamaoka; Kenji Yoshino; Taketo Yamada; Chiyoko Idehara; Mohammad O. Hoque; Maki Moritani; Katsuhiko Yoshimoto; Jun ich Hata; Mitsuo Itakura

doi:10.1006/bbrc.2000.3813

Diabetes and tumor formation in transgenic mice expressing Reg I

Takashi Yamaoka, Kenji Yoshino, Taketo Yamada, Chiyoko Idehara, Mohammad O. Hoque, Maki Moritani, Katsuhiko Yoshimoto, Jun ich Hata, Mitsuo Itakura

Research output: Contribution to journal › Article › peer-review

25 Scopus citations

Abstract

To examine the effect of overexpressed regenerating gene (Reg) I on pancreatic β-cells, we generated transgenic mice expressing Reg I in islets (Reg-Tg mice). Three lines of Reg-Tg mice were established. In line-1 Reg-Tg mice, the expression level of Reg I mRNA in islets was 7 times higher than those in lines 2 and 3 of Reg-Tg mice, and line 1 mice developed diabetes by apoptosis of β-cells, as well as various malignant tumors. In addition to the decrease in β-cells, compensatory islet regeneration and proliferation of ductal epithelial cells were observed in llne-1 Reg-Tg mice. Because Reg I protein was secreted primarily into pancreatic ducts from acinar cells, it may primarily stimulate the proliferation of ductal epithelial cells, and not β-cells, and their differentiation into islets. Moreover, the tumor-promoting activity of Reg I protein should be considered for its possible clinical applications. (C) 2000 Academic Press.

Original language	English (US)
Pages (from-to)	368-376
Number of pages	9
Journal	Biochemical and Biophysical Research Communications
Volume	278
Issue number	2
DOIs	https://doi.org/10.1006/bbrc.2000.3813
State	Published - Nov 19 2000
Externally published	Yes

Keywords

Apoptosis
Neoplasm
Pancreatic islet
Reg I
Regeneration
Transgenic mouse

ASJC Scopus subject areas

Biophysics
Biochemistry
Molecular Biology
Cell Biology

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10.1006/bbrc.2000.3813

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title = "Diabetes and tumor formation in transgenic mice expressing Reg I",

abstract = "To examine the effect of overexpressed regenerating gene (Reg) I on pancreatic β-cells, we generated transgenic mice expressing Reg I in islets (Reg-Tg mice). Three lines of Reg-Tg mice were established. In line-1 Reg-Tg mice, the expression level of Reg I mRNA in islets was 7 times higher than those in lines 2 and 3 of Reg-Tg mice, and line 1 mice developed diabetes by apoptosis of β-cells, as well as various malignant tumors. In addition to the decrease in β-cells, compensatory islet regeneration and proliferation of ductal epithelial cells were observed in llne-1 Reg-Tg mice. Because Reg I protein was secreted primarily into pancreatic ducts from acinar cells, it may primarily stimulate the proliferation of ductal epithelial cells, and not β-cells, and their differentiation into islets. Moreover, the tumor-promoting activity of Reg I protein should be considered for its possible clinical applications. (C) 2000 Academic Press.",

keywords = "Apoptosis, Neoplasm, Pancreatic islet, Reg I, Regeneration, Transgenic mouse",

author = "Takashi Yamaoka and Kenji Yoshino and Taketo Yamada and Chiyoko Idehara and Hoque, {Mohammad O.} and Maki Moritani and Katsuhiko Yoshimoto and Hata, {Jun ich} and Mitsuo Itakura",

note = "Funding Information: This study was supported in part by a grant from Otsuka Pharmaceutical Factory, Inc. to the Otsuka Department of Molecular Nutrition, School of Medicine, University of Tokushima.",

year = "2000",

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doi = "10.1006/bbrc.2000.3813",

language = "English (US)",

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T1 - Diabetes and tumor formation in transgenic mice expressing Reg I

AU - Yamaoka, Takashi

AU - Yoshino, Kenji

AU - Yamada, Taketo

AU - Idehara, Chiyoko

AU - Hoque, Mohammad O.

AU - Moritani, Maki

AU - Yoshimoto, Katsuhiko

AU - Hata, Jun ich

AU - Itakura, Mitsuo

N1 - Funding Information: This study was supported in part by a grant from Otsuka Pharmaceutical Factory, Inc. to the Otsuka Department of Molecular Nutrition, School of Medicine, University of Tokushima.

PY - 2000/11/19

Y1 - 2000/11/19

N2 - To examine the effect of overexpressed regenerating gene (Reg) I on pancreatic β-cells, we generated transgenic mice expressing Reg I in islets (Reg-Tg mice). Three lines of Reg-Tg mice were established. In line-1 Reg-Tg mice, the expression level of Reg I mRNA in islets was 7 times higher than those in lines 2 and 3 of Reg-Tg mice, and line 1 mice developed diabetes by apoptosis of β-cells, as well as various malignant tumors. In addition to the decrease in β-cells, compensatory islet regeneration and proliferation of ductal epithelial cells were observed in llne-1 Reg-Tg mice. Because Reg I protein was secreted primarily into pancreatic ducts from acinar cells, it may primarily stimulate the proliferation of ductal epithelial cells, and not β-cells, and their differentiation into islets. Moreover, the tumor-promoting activity of Reg I protein should be considered for its possible clinical applications. (C) 2000 Academic Press.

AB - To examine the effect of overexpressed regenerating gene (Reg) I on pancreatic β-cells, we generated transgenic mice expressing Reg I in islets (Reg-Tg mice). Three lines of Reg-Tg mice were established. In line-1 Reg-Tg mice, the expression level of Reg I mRNA in islets was 7 times higher than those in lines 2 and 3 of Reg-Tg mice, and line 1 mice developed diabetes by apoptosis of β-cells, as well as various malignant tumors. In addition to the decrease in β-cells, compensatory islet regeneration and proliferation of ductal epithelial cells were observed in llne-1 Reg-Tg mice. Because Reg I protein was secreted primarily into pancreatic ducts from acinar cells, it may primarily stimulate the proliferation of ductal epithelial cells, and not β-cells, and their differentiation into islets. Moreover, the tumor-promoting activity of Reg I protein should be considered for its possible clinical applications. (C) 2000 Academic Press.

KW - Apoptosis

KW - Neoplasm

KW - Pancreatic islet

KW - Reg I

KW - Regeneration

KW - Transgenic mouse

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Diabetes and tumor formation in transgenic mice expressing Reg I

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