12-h clock regulation of genetic information flow by XBP1s

Pan, Yinghong and Ballance, Heather and Meng, Huan and Gonzalez, Naomi and Kim, Sam-Moon and Abdurehman, Leymaan and York, Brian and Chen, Xi and Schnytzer, Yisrael and Levy, Oren and Dacso, Clifford C. and McClung, Colleen A. and O’Malley, Bert W. and Liu, Silvia and Zhu, Bokai and Kramer, Achim (2020) 12-h clock regulation of genetic information flow by XBP1s. PLOS Biology, 18 (1). e3000580. ISSN 1545-7885

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Abstract

Our group recently characterized a cell-autonomous mammalian 12-h clock independent from the circadian clock, but its function and mechanism of regulation remain poorly understood. Here, we show that in mouse liver, transcriptional regulation significantly contributes to the establishment of 12-h rhythms of mRNA expression in a manner dependent on Spliced Form of X-box Binding Protein 1 (XBP1s). Mechanistically, the motif stringency of XBP1s promoter binding sites dictates XBP1s’s ability to drive 12-h rhythms of nascent mRNA transcription at dawn and dusk, which are enriched for basal transcription regulation, mRNA processing and export, ribosome biogenesis, translation initiation, and protein processing/sorting in the Endoplasmic Reticulum (ER)-Golgi in a temporal order consistent with the progressive molecular processing sequence described by the central dogma information flow (CEDIF). We further identified GA-binding proteins (GABPs) as putative novel transcriptional regulators driving 12-h rhythms of gene expression with more diverse phases. These 12-h rhythms of gene expression are cell autonomous and evolutionarily conserved in marine animals possessing a circatidal clock. Our results demonstrate an evolutionarily conserved, intricate network of transcriptional control of the mammalian 12-h clock that mediates diverse biological pathways. We speculate that the 12-h clock is coopted to accommodate elevated gene expression and processing in mammals at the two rush hours, with the particular genes processed at each rush hour regulated by the circadian and/or tissue-specific pathways.

Item Type: Article
Subjects: Opene Prints > Biological Science
Depositing User: Managing Editor
Date Deposited: 25 Jan 2023 05:43
Last Modified: 17 Jan 2024 04:13
URI: http://geographical.go2journals.com/id/eprint/1146

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