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BMAL1-Driven Tissue Clocks Respond Independently to Light to Maintain Homeostasis
Author(s) -
Patrick-Simon Welz,
Valentina M. Zinna,
Aikaterini Symeonidi,
Kevin B. Koronowski,
Kenichiro Kinouchi,
Jacob G. Smith,
Inés Marín,
Andrés CastellanosMartín,
Stephen Furrow,
Fernando Cruz Aragon,
Georgiana Crainiciuc,
Neus Prats,
Juan Martín Caballero,
Andrés Hidalgo,
Paolo Sassone–Corsi,
Salvador Aznar Benitah
Publication year - 2019
Publication title -
cell
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 26.304
H-Index - 776
eISSN - 1097-4172
pISSN - 0092-8674
DOI - 10.1016/j.cell.2019.05.009
Subject(s) - biology , homeostasis , microbiology and biotechnology
Circadian rhythms control organismal physiology throughout the day. At the cellular level, clock regulation is established by a self-sustained Bmal1-dependent transcriptional oscillator network. However, it is still unclear how different tissues achieve a synchronized rhythmic physiology. That is, do they respond independently to environmental signals, or require interactions with each other to do so? We show that unexpectedly, light synchronizes the Bmal1-dependent circadian machinery in single tissues in the absence of Bmal1 in all other tissues. Strikingly, light-driven tissue autonomous clocks occur without rhythmic feeding behavior and are lost in constant darkness. Importantly, tissue-autonomous Bmal1 partially sustains homeostasis in otherwise arrhythmic and prematurely aging animals. Our results therefore support a two-branched model for the daily synchronization of tissues: an autonomous response branch, whereby light entrains circadian clocks without any commitment of other Bmal1-dependent clocks, and a memory branch using other Bmal1-dependent clocks to "remember" time in the absence of external cues.

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