| Literature DB >> 29271671 |
Tomomi Nakao1, Akira Kohsaka1, Tsuyoshi Otsuka1, Zaw Lin Thein1, Hue Thi Le1, Hidefumi Waki2, Sabine S Gouraud3, Hayato Ihara4, Masako Nakanishi5, Fuyuki Sato5, Yasuteru Muragaki5, Masanobu Maeda1.
Abstract
The daily rhythm of glucose metabolism is governed by the circadian clock, which consists of cell-autonomous clock machineries residing in nearly every tissue in the body. Disruption of these clock machineries either environmentally or genetically induces the dysregulation of glucose metabolism. Although the roles of clock machineries in the regulation of glucose metabolism have been uncovered in major metabolic tissues, such as the pancreas, liver, and skeletal muscle, it remains unknown whether clock function in non-major metabolic tissues also affects systemic glucose metabolism. Here, we tested the hypothesis that disruption of the clock machinery in the heart might also affect systemic glucose metabolism, because heart function is known to be associated with glucose tolerance. We examined glucose and insulin tolerance as well as heart phenotypes in mice with heart-specific deletion of Bmal1, a core clock gene. Bmal1 deletion in the heart not only decreased heart function but also led to systemic insulin resistance. Moreover, hyperglycemia was induced with age. Furthermore, heart-specific Bmal1-deficient mice exhibited decreased insulin-induced phosphorylation of Akt in the liver, thus indicating that Bmal1 deletion in the heart causes hepatic insulin resistance. Our findings revealed an unexpected effect of the function of clock machinery in a non-major metabolic tissue, the heart, on systemic glucose metabolism in mammals.Entities:
Keywords: Circadian clock; glucose metabolism; heart; liver
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Year: 2017 PMID: 29271671 DOI: 10.1080/07420528.2017.1415922
Source DB: PubMed Journal: Chronobiol Int ISSN: 0742-0528 Impact factor: 2.877