REV-ERBα and REV-ERBβ function as key factors regulating Mammalian Circadian Output

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Ryosuke Ikeda
Yoshiki Tsuchiya
Nobuya Koike
Yasuhiro Umemura
Hitoshi Inokawa
Ryutaro Ono
Maho Inoue
Yuh Sasawaki
Tess Grieten
Naoki Okubo
Kazuya Ikoma
Hiroyoshi Fujiwara
Toshikazu Kubo
Kazuhiro Yagita
机构
[1] Kyoto Prefectural University of Medicine,Department of Physiology and Systems Bioscience
[2] Kawaramachi-Hirokoji,Department of Orthopaedics
[3] Kyoto Prefectural University of Medicine,undefined
[4] Kawaramachi-Hirokoji,undefined
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The circadian clock regulates behavioural and physiological processes in a 24-h cycle. The nuclear receptors REV-ERBα and REV-ERBβ are involved in the cell-autonomous circadian transcriptional/translational feedback loops as transcriptional repressors. A number of studies have also demonstrated a pivotal role of REV-ERBs in regulation of metabolic, neuronal, and inflammatory functions including bile acid metabolism, lipid metabolism, and production of inflammatory cytokines. Given the multifunctional role of REV-ERBs, it is important to elucidate the mechanism through which REV-ERBs exert their functions. To this end, we established a Rev-erbα/Rev-erbβ double-knockout mouse embryonic stem (ES) cell model and analyzed the circadian clock and clock-controlled output gene expressions. A comprehensive mRNA-seq analysis revealed that the double knockout of both Rev-erbα and Rev-erbβ does not abrogate expression rhythms of E-box-regulated core clock genes but drastically changes a diverse set of other rhythmically-expressed output genes. Of note, REV-ERBα/β deficiency does not compromise circadian expression rhythms of PER2, while REV-ERB target genes, Bmal1 and Npas2, are significantly upregulated. This study highlight the relevance of REV-ERBs as pivotal output mediators of the mammalian circadian clock.
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