Slowpoke functions in circadian output cells to regulate rest: Activity rhythms

Slowpoke functions in circadian output cells to regulate rest: Activity rhythms

The circadian system produces similar to 24-hr oscillations in behavioral and physiological processes to ensure that they occur at optimal times of day and in the correct temporal order. At its core, the circadian system is composed of dedicated central clock neurons that keep time through a cell-au...

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Veröffentlicht in:PloS one 2021-03, Vol.16 (3), p.e0249215-e0249215, Article 0249215
Hauptverfasser: Ruiz, Daniela, Bajwa, Saffia T., Vanani, Naisarg, Bajwa, Tanvir A., Cavanaugh, Daniel J.
Format: Artikel
Sprache:eng
Schlagworte:
Behavior
Biology
Biology and Life Sciences
Circadian rhythm
Circadian rhythms
Clocks
Fasting
Gene expression
Insects
Insulin
Mammals
Multidisciplinary Sciences
Neuropeptides
Peptides
Science & Technology
Science & Technology - Other Topics
Social Sciences
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Zusammenfassung:The circadian system produces similar to 24-hr oscillations in behavioral and physiological processes to ensure that they occur at optimal times of day and in the correct temporal order. At its core, the circadian system is composed of dedicated central clock neurons that keep time through a cell-autonomous molecular clock. To produce rhythmic behaviors, time-of-day information generated by clock neurons must be transmitted across output pathways to regulate the downstream neuronal populations that control the relevant behaviors. An understanding of the manner through which the circadian system enacts behavioral rhythms therefore requires the identification of the cells and molecules that make up the output pathways. To that end, we recently characterized the Drosophila pars intercerebralis (PI) as a major circadian output center that lies downstream of central clock neurons in a circuit controlling rest:activity rhythms. We have conducted single-cell RNA sequencing (scRNAseq) to identify potential circadian output genes expressed by PI cells, and used cell-specific RNA interference (RNAi) to knock down expression of similar to 40 of these candidate genes selectively within subsets of PI cells. We demonstrate that knockdown of the slowpoke (slo) potassium channel in PI cells reliably decreases circadian rest:activity rhythm strength. Interestingly, slo mutants have previously been shown to have aberrant rest:activity rhythms, in part due to a necessary function of slo within central clock cells. However, rescue of slo in all clock cells does not fully reestablish behavioral rhythms, indicating that expression in non-clock neurons is also necessary. Our results demonstrate that slo exerts its effects in multiple components of the circadian circuit, including PI output cells in addition to clock neurons, and we hypothesize that it does so by contributing to the generation of daily neuronal activity rhythms that allow for the propagation of circadian information throughout output circuits.
ISSN:1932-6203
1932-6203
DOI:10.1371/journal.pone.0249215