Scientists Unveil Ticking of Nature's Simplest Clock

National Institutes of Natural Sciences

Aichi, Japan--Researchers from the Institute for Molecular Science (IMS)/SOKENDAI and Kyushu University have uncovered the molecular mechanism that drives the "ticking" of the circadian clock in cyanobacteria. Their study reveals how a clock protein called KaiC controls chemical reactions with remarkable precision, acting like the hand of a clock that waits, then moves at just the right moment. The findings were published in PNAS Nexus on April 28, 2025.

To adapt to Earth's daily rotation, most living organisms, from simple, single-celled bacteria to complex, multicellular mammals, have evolved internal timekeeping systems known as circadian clocks. Among all known species, only cyanobacteria possess a circadian clock system that scientists have been able to fully reproduce in a test tube. This system involves three proteins, KaiA, KaiB, and KaiC. When mixed in a test tube, KaiC undergoes a cycle of phosphorylation and dephosphorylation, a rhythmic attachment and detachment of phosphate groups that repeats every 24 hours, just like a clock (Figure 1A). Despite decades of study, a key mystery remained. How exactly does the phosphate attach to KaiC? In other words, what drives the motion of the clock's hand?

To answer this question, the research team, led by Assistant Professor Yoshihiko Furuike and Professor Shuji Akiyama from IMS/ SOKENDAI, and Associate Professor Toshifumi Mori from Kyushu University focused on KaiC in isolation, without KaiA and KaiB. This simplified system enabled direct observation of the phosphorylation process. Contrary to previous assumptions, they discovered that even alone, KaiC can slowly bind phosphate, indicating that the fundamental "ticking" of the clock resides within KaiC itself (Figure 1B).

Using the structural data of KaiC obtained at near-atomic resolution, the team simulated the chemical reaction of phosphorylation through molecular dynamics and quantum chemical simulations. This method allowed them to observe how a phosphate group gradually approaches and binds to KaiC (Figure 1C).

The team found that subtle shifts in the arrangement of certain amino acids, specifically glutamate and arginine residues, serve as molecular triggers. These residues effectively control whether the phosphate group can bind, thereby pausing or permitting the reaction like a timed gate. In other words, KaiC holds the clock hand steady until the precise moment it should tick.

The mechanism discovered in this study is not limited to cyanobacteria. Many organisms, including humans, rely on phosphorylation to regulate their internal clocks. This research thus provides fundamental insights into the universal logic of biological timekeeping.

Moreover, since phosphorylation is related to various diseases, understanding how proteins control the timing of chemical reactions may have far-reaching applications in biomedicine and drug design. While this study focused on the phosphorylation process, the dephosphorylation remains less well understood and is a key topic for future investigation.

Glossary

  1. Cyanobacteria: Oxygen-producing bacteria that perform photosynthesis. They are known for having the simplest circadian clock system studied to date.
  2. Circadian clock: An internal biological system that regulates daily rhythms in living organisms, such as sleep, metabolism, and photosynthesis. Found in organisms from bacteria to humans, circadian clocks follow a roughly 24-hour cycle and can synchronize with environmental cues.
  3. Phosphorylation / Dephosphorylation: The attachment or removal of a phosphate group to or from a protein. These processes often change the structure of proteins, thereby switching or modulating their functions.
  4. Simulation of chemical reactions: A computational method that simulates the movement of atoms and molecules over time. It is used to visualize chemical reactions that are difficult to observe experimentally.

Information of the paper:

Authors: Yoshihiko Furuike, Yasuhiro Onoue, Shinji Saito, Toshifumi Mori, Shuji Akiyama

Journal Name: PNAS Nexus

Journal Title: "The priming phosphorylation of KaiC is activated by the release of its autokinase autoinhibition"

DOI: 10.1093/pnasnexus/pgaf136

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