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Functional adenosine triphosphate‐sensitive potassium channel is required in high‐carbohydrate diet‐induced increase in β‐cell mass
Author(s) -
Murase Masatoshi,
Seino Yusuke,
Maekawa Ryuya,
Iida Atsushi,
Hosokawa Kaori,
Hayami Tomohide,
Tsunekawa Shin,
Hamada Yoji,
Yokoi Norihide,
Seino Susumu,
Hayashi Yoshitaka,
Arima Hiroshi
Publication year - 2019
Publication title -
journal of diabetes investigation
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.089
H-Index - 50
eISSN - 2040-1124
pISSN - 2040-1116
DOI - 10.1111/jdi.12907
Subject(s) - medicine , adenosine triphosphate , potassium channel , diabetes mellitus , adenosine , carbohydrate metabolism , potassium , carbohydrate , type 2 diabetes , endocrinology , chemistry , organic chemistry
Abstract Aims/Introduction A high‐carbohydrate diet is known to increase insulin secretion and induce obesity. However, whether or not a high‐carbohydrate diet affects β‐cell mass ( BCM ) has been little investigated. Materials and Methods Both wild‐type ( WT ) mice and adenosine triphosphate‐sensitive potassium channel‐deficient (Kir6.2 KO ) mice were fed normal chow or high‐starch ( ST ) diets for 22 weeks. BCM and the numbers of islets were analyzed by immunohistochemistry, and gene expression levels in islets were investigated by quantitative real‐time reverse transcription polymerase chain reaction. MIN 6‐K8 β‐cells were stimulated in solution containing various concentrations of glucose combined with nifedipine and glimepiride, and gene expression was analyzed. Results Both WT and Kir6.2 KO mice fed ST showed hyperinsulinemia and body weight gain. BCM , the number of islets and the expression levels of cyclinD2 messenger ribonucleic acid were increased in WT mice fed ST compared with those in WT mice fed normal chow. In contrast, no significant difference in BCM , the number of islets or the expression levels of cyclinD2 messenger ribonucleic acid were observed between Kir6.2 KO mice fed normal chow and those fed ST . Incubation of MIN 6‐K8 β‐cells in high‐glucose media or with glimepiride increased cyclinD2 expression, whereas nifedipine attenuated a high‐glucose‐induced increase in cyclinD2 expression. Conclusions These results show that a high‐starch diet increases BCM in an adenosine triphosphate‐sensitive potassium channel‐dependent manner, which is mediated through upregulation of cyclinD2 expression.

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