| Literature DB >> 35507871 |
Yoshihiko Furuike1,2, Atsushi Mukaiyama1,2, Shin-Ichi Koda3, Damien Simon1,2, Dongyan Ouyang1, Kumiko Ito-Miwa4, Shinji Saito3, Eiki Yamashita5, Taeko Nishiwaki-Ohkawa6,7, Kazuki Terauchi8,9, Takao Kondo4, Shuji Akiyama1,2.
Abstract
KaiC is a dual adenosine triphosphatase (ATPase), with one active site in its N-terminal domain and another in its C-terminal domain, that drives the circadian clock system of cyanobacteria through sophisticated coordination of the two sites. To elucidate the coordination mechanism, we studied the contribution of the dual-ATPase activities in the ring-shaped KaiC hexamer and these structural bases for activation and inactivation. At the N-terminal active site, a lytic water molecule is sequestered between the N-terminal domains, and its reactivity to adenosine triphosphate (ATP) is controlled by the quaternary structure of the N-terminal ring. The C-terminal ATPase activity is regulated mostly by water-incorporating voids between the C-terminal domains, and the size of these voids is sensitive to phosphoryl modification of S431. The up-regulatory effect on the N-terminal ATPase activity inversely correlates with the affinity of KaiC for KaiB, a clock protein constitutes the circadian oscillator together with KaiC and KaiA, and the complete dissociation of KaiB from KaiC requires KaiA-assisted activation of the dual ATPase. Delicate interactions between the N-terminal and C-terminal rings make it possible for the components of the dual ATPase to work together, thereby driving the assembly and disassembly cycle of KaiA and KaiB.Entities:
Keywords: ATPase; KaiC; circadian clock; cyanobacteria; structure
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Year: 2022 PMID: 35507871 PMCID: PMC9171630 DOI: 10.1073/pnas.2119627119
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 12.779