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Dopamine and GPCR-mediated modulation of DN1 clock neurons gates the circadian timing of sleep.


ABSTRACT: The metronome-like circadian regulation of sleep timing must still adapt to an uncertain environment. Recent studies in Drosophila indicate that neuromodulation not only plays a key role in clock neuron synchronization but also affects interactions between the clock network and brain sleep centers. We show here that the targets of neuromodulators, G Protein Coupled Receptors (GPCRs), are highly enriched in the fly brain circadian clock network. Single-cell sequencing indicates that they are not only enriched but also differentially expressed and contribute to clock neuron identity. We generated a comprehensive guide library to mutagenize individual GPCRs in specific neurons and verified the strategy by introducing a targeted sequencing approach. Combined with a behavioral screen, the mutagenesis strategy revealed a role of dopamine in sleep regulation by identifying two dopamine receptors and a clock neuron subpopulation that gate the timing of sleep.

SUBMITTER: Schlichting M 

PROVIDER: S-EPMC9407311 | biostudies-literature | 2022 Aug

REPOSITORIES: biostudies-literature

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Dopamine and GPCR-mediated modulation of DN1 clock neurons gates the circadian timing of sleep.

Schlichting Matthias M   Richhariya Shlesha S   Herndon Nicholas N   Ma Dingbang D   Xin Jason J   Lenh William W   Abruzzi Katharine K   Rosbash Michael M  

Proceedings of the National Academy of Sciences of the United States of America 20220815 34


The metronome-like circadian regulation of sleep timing must still adapt to an uncertain environment. Recent studies in <i>Drosophila</i> indicate that neuromodulation not only plays a key role in clock neuron synchronization but also affects interactions between the clock network and brain sleep centers. We show here that the targets of neuromodulators, G Protein Coupled Receptors (GPCRs), are highly enriched in the fly brain circadian clock network. Single-cell sequencing indicates that they a  ...[more]

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