Targeted disruption of the Chop gene delays endoplasmic reticulum stress–mediated diabetes

Oyadomari, Seiichi; Koizumi, Akio; Takeda, Kiyoshi; Gotoh, Tomomi; Akira, Shizuo; Araki, Eiichi; Mori, Masataka

doi:10.1172/jci0214550

articleJournal of Clinical InvestigationFeb 15, 2002Closed access

Targeted disruption of the Chop gene delays endoplasmic reticulum stress–mediated diabetes

SOSeiichi Oyadomari AKAkio KoizumiKTKiyoshi TakedaTGTomomi Gotoh SAShizuo Akira

Laboratory of Molecular Genetics · Kumamoto University · +2 more institutions

Indexed incrossrefdoaj

Abstract

Overload of pancreatic β cells in conditions such as hyperglycemia, obesity, and long-term treatment with sulfonylureas leads to β cell exhaustion and type 2 diabetes. Because β cell mass declines under these conditions, apparently as a result of apoptosis, we speculated that overload kills β cells as a result of endoplasmic reticulum (ER) stress. The Akita mouse, which carries a conformation-altering missense mutation (Cys96Tyr) in Insulin 2, likewise exhibits hyperglycemia and a reduced β cell mass. In the development of diabetes in Akita mice, mRNAs for the ER chaperone Bip and the ER stress–associated apoptosis factor Chop were induced in the pancreas. Overexpression of the mutant insulin in mouse MIN6 β…

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Authors

7

SO
Seiichi OyadomariCorresponding
Laboratory of Molecular Genetics, Kumamoto University
AK
Akio Koizumi
Kyoto University
KT
Kiyoshi Takeda
The University of Osaka
TG
Tomomi Gotoh
Laboratory of Molecular Genetics
SA
Shizuo Akira
The University of Osaka

Topics & keywords

Topics

Keywords

CHOP
Endoplasmic reticulum
Unfolded protein response
Chemical chaperone
Apoptosis
Endocrinology
Internal medicine
Missense mutation

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Funding

LT
La Trobe University