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research article

Topology and dynamics of the zebrafish segmentation clock core circuit

Schröter, Christian
•
Ares, Saúl
•
Morelli, Luis G.
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2012
PLoS Biology

During vertebrate embryogenesis, the rhythmic and sequential segmentation of the body axis is regulated by an oscillating genetic network termed the segmentation clock. We describe a new dynamic model for the core pace-making circuit of the zebrafish segmentation clock based on a systematic biochemical investigation of the network's topology and precise measurements of somitogenesis dynamics in novel genetic mutants. We show that the core pace-making circuit consists of two distinct negative feedback loops, one with Her1 homodimers and the other with Her7:Hes6 heterodimers, operating in parallel. To explain the observed single and double mutant phenotypes of her1, her7, and hes6 mutant embryos in our dynamic model, we postulate that the availability and effective stability of the dimers with DNA binding activity is controlled in a "dimer cloud" that contains all possible dimeric combinations between the three factors. This feature of our model predicts that Hes6 protein levels should oscillate despite constant hes6 mRNA production, which we confirm experimentally using novel Hes6 antibodies. The control of the circuit's dynamics by a population of dimers with and without DNA binding activity is a new principle for the segmentation clock and may be relevant to other biological clocks and transcriptional regulatory networks. © 2012 Schröter et al.

  • Details
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Type
research article
DOI
10.1371/journal.pbio.1001364
Web of Science ID

WOS:000307161000008

Scopus ID

2-s2.0-84875566370

Author(s)
Schröter, Christian
Ares, Saúl
Morelli, Luis G.
Isakova, Alina  
Hens, Korneel  
Soroldoni, Daniele  
Gajewski, Martin
Jülicher, Frank
Maerkl, Sebastian J.  
Deplancke, Bart  
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Date Issued

2012

Published in
PLoS Biology
Volume

10

Issue

7

Article Number

e1001364

Subjects

animal experiment

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animal tissue

•

Article

•

basic helix loop helix transcription factor

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controlled study

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Danio rerio

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Developmental biology

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embryo

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embryo development

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embryonic structures

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embryo segmentation

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gene

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her1 gene

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her6 gene

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her7 gene

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homodimer

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messenger RNA

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messenger RNA synthesis

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molecular clock

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Molecular dynamics

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mutant

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nonhuman

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phenotype

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Prediction

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protein antibody

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protein DNA binding

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protein function

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protein stability

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somitogenesis

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transcription factor Her1

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transcription factor Her6

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transcription factor Her6 antibody

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transcription factor Her7

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transcription regulation

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unclassified drug

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Vertebrata

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zebra fish

Editorial or Peer reviewed

REVIEWED

Written at

EPFL

EPFL units
LBNC  
UPDEPLA  
UPOATES  
Available on Infoscience
May 30, 2017
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/137755
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