Literature DB >> 31539528

Transcription-based circadian mechanism controls the duration of molecular clock states in response to signaling inputs.

Sofia Almeida1, Madalena Chaves2, Franck Delaunay3.   

Abstract

The molecular oscillator of the mammalian circadian clock consists in a dynamical network of genes and proteins whose main regulatory mechanisms occur at the transcriptional level. From a dynamical point of view, the mechanisms leading to an oscillatory solution with an orderly protein peak expression and a clear day/night phase distinction remain unclear. Our goal is to identify the essential interactions needed to generate phase opposition between the activating CLOCK:BMAL1 and the repressing PER:CRY complexes and to better distinguish these two main clock molecular phases relating to rest/activity and fast/feeding cycles. To do this, we develop a transcription-based mathematical model centered on linear combinations of the clock controlled elements (CCEs): E-box, R-box and D-box. Each CCE is responsive to activators and repressors. After model calibration with single-cell data, we explore entrainment and period tuning via interplay with metabolism. Variation of the PER degradation rate γp, relating to the tau mutation, results in asymmetric changes in the duration of the different clock molecular phases. Time spent at the state of high PER/PER:CRY decreases with γp, while time spent at the state of high BMAL1 and CRY1, both proteins with activity in promoting insulin sensitivity, remains constant. This result suggests a possible mechanism behind the altered metabolism of tau mutation animals. Furthermore, we expose the clock system to two regulatory inputs, one relating to the fast/feeding cycle and the other to the light-dependent synchronization signaling. We observe the phase difference between these signals to also affect the relative duration of molecular clock states. Simulated circadian misalignment, known to correlate with insulin resistance, leads to decreased duration of BMAL1 expression. Our results reveal a possible mechanism for clock-controlled metabolic homeostasis, whereby the circadian clock controls the relative duration of different molecular (and metabolic) states in response to signaling inputs.
Copyright © 2019 Elsevier Ltd. All rights reserved.

Entities:  

Keywords:  Calibration; Circadian alignment; Mammalian clock model; Transcriptional regulation; tau mutation

Mesh:

Substances:

Year:  2019        PMID: 31539528     DOI: 10.1016/j.jtbi.2019.110015

Source DB:  PubMed          Journal:  J Theor Biol        ISSN: 0022-5193            Impact factor:   2.691


  8 in total

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2.  Cycle dynamics and synchronization in a coupled network of peripheral circadian clocks.

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Journal:  Interface Focus       Date:  2022-04-15       Impact factor: 4.661

3.  Combined multiple transcriptional repression mechanisms generate ultrasensitivity and oscillations.

Authors:  Eui Min Jeong; Yun Min Song; Jae Kyoung Kim
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Authors:  Xinhui Wu; I Sophie T Bos; Thomas M Conlon; Meshal Ansari; Vicky Verschut; Luke van der Koog; Lars A Verkleij; Angela D'Ambrosi; Aleksey Matveyenko; Herbert B Schiller; Melanie Königshoff; Martina Schmidt; Loes E M Kistemaker; Ali Önder Yildirim; Reinoud Gosens
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5.  Data-driven modelling captures dynamics of the circadian clock of Neurospora crassa.

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6.  Live-cell imaging of circadian clock protein dynamics in CRISPR-generated knock-in cells.

Authors:  Christian H Gabriel; Marta Del Olmo; Amin Zehtabian; Marten Jäger; Silke Reischl; Hannah van Dijk; Carolin Ulbricht; Asylkhan Rakhymzhan; Thomas Korte; Barbara Koller; Astrid Grudziecki; Bert Maier; Andreas Herrmann; Raluca Niesner; Tomasz Zemojtel; Helge Ewers; Adrián E Granada; Hanspeter Herzel; Achim Kramer
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7.  Nonlinear phenomena in models of the circadian clock.

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Review 8.  Circadian Misalignment and Metabolic Disorders: A Story of Twisted Clocks.

Authors:  Aurore Woller; Didier Gonze
Journal:  Biology (Basel)       Date:  2021-03-10
  8 in total

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