Two coupled circadian oscillations regulate Bmal1-ELuc and Per2-SLR2 expression in the mouse suprachiasmatic nucleus

Oct 5, 2018Scientific reports

Two linked daily rhythms control Bmal1 and Per2 gene activity in the mouse brain's internal clock

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Abstract

Circadian rhythms of Bmal1 and Per2 in the mouse suprachiasmatic nucleus show distinct phase relationships under different conditions.

  • In neonatal SCN, phase relationships between Bmal1 and Per2 rhythms significantly changed during culture.
  • Medium exchange caused phase shifts in Bmal1 rhythms but did not affect Per2 rhythms, leading to temporal dissociation.
  • In adult SCN, phase relationships between the two rhythms remained constant for at least 20 cycles.
  • The amplitude of phase shifts in Bmal1 rhythms was significantly reduced in adults, while a phase shift developed in Per2 rhythms.
  • Circadian periods were not systematically affected by medium exchange in either rhythm, regardless of age.
  • Tetrodotoxin enhanced phase responses in both rhythms but eliminated phase dependency, and lengthened circadian periods irrespective of administration timing.

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Key numbers

10.17 ± 0.34 h in the first 10 cycles vs. 7.66 ± 0.75 h in the last 10 cycles
Phase Difference Decrease
Phase difference (ψ) between Bmal1 and Per2 rhythms in neonatal SCN slices.
0.22 ± 0.05 h
Circadian Period Difference
Mean free-running circadian period difference calculated from regression lines.
7.0 ± 2.3 h vs. 4.0 ± 1.8 h
Medium Exchange Phase Shift
Magnitude of phase shift in response to medium exchange in neonatal vs. adult SCN.

Full Text

What this is

  • This research investigates the circadian rhythms of clock genes Bmal1 and Per2 in the mouse suprachiasmatic nucleus (SCN).
  • Using dual bioluminescence reporters, the study monitors these rhythms simultaneously in neonatal and adult SCN slices.
  • Key findings include the dissociation of these rhythms in neonatal SCN slices and their distinct responses to medium exchange.

Essence

  • Bmal1 and Per2 circadian rhythms in the SCN are regulated by different oscillators, showing developmental dissociation in neonatal mice. Medium exchange affects these rhythms differently based on age.

Key takeaways

  • Neonatal SCN slices show dissociation between Bmal1 and Per2 rhythms, while adult SCN slices maintain a stable phase relationship. This indicates that developmental stage influences the regulation of circadian rhythms.
  • Medium exchange induces phase shifts in Bmal1 rhythms in neonatal SCN but not in adult SCN. The phase shifts are larger in neonatal mice, suggesting a heightened sensitivity to environmental changes.
  • Tetrodotoxin treatment enhances phase shifts in both rhythms but disrupts their phase dependency. This indicates that neural communication within the SCN is crucial for maintaining coherence.

Caveats

  • The study primarily uses cultured SCN slices, which may not fully replicate in vivo conditions. This limits the generalizability of the findings to whole organisms.
  • The mechanisms behind the observed phase shifts and dissociation remain unclear, necessitating further research to understand the underlying processes.

Definitions

  • circadian rhythm: A biological process that displays an endogenous oscillation of about 24 hours, influenced by external cues like light.

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