Regulation of the Activity and Cellular Localization of the Circadian Clock Protein FRQ

Cha, Joonseok; Yuan, Haiyan; Liu, Yi

doi:10.1074/jbc.m111.219782

Cited by 44 publications

(51 citation statements)

References 54 publications

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“…Moreover, CK1a is activated by recruitment to FRQ. In this way, a single molecule of bound CK1a could phosphorylate in cis a large number of sites that are distributed all over the intrinsically disordered polypeptide chain of FRQ and also WCC that is recruited to the FFC 16,17,29 .…”

Section: Resultsmentioning

confidence: 99%

“…FRH is essential for the viability of Neurospora owing to its function in RNA metabolism 14 . In addition, FRH has been implicated in a variety of non-essential, clock-related functions: FRH is crucial for cytoplasmic localization and turnover of FRQ 15,16 , and also for the interaction of FRQ with the circadian transcription activator White Collar Complex (WCC) 15,17 . Furthermore, it was reported that FRH mediates turnover of frq RNA by committing the messenger for degradation by the exosome 14 .…”

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confidence: 99%

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The RNA helicase FRH is an ATP-dependent regulator of CK1a in the circadian clock of Neurospora crassa

et al. 2014

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The Neurospora clock protein FRQ forms a complex with casein kinase 1a (CK1a) and FRH, a DEAD box-containing RNA helicase with a clock-independent essential function in RNA metabolism. In the course of a circadian period, FRQ is progressively hyperphosphorylated and eventually degraded. Timed hyperphosphorylation of FRQ is crucial for timekeeping of the clock. Here we show that the ATPase activity of FRH attenuates the kinetics of CK1a-mediated hyperphosphorylation of FRQ. Hyperphosphorylation of FRQ is strictly dependent on site-specific recruitment of a CK1a molecule that is activated upon binding. The FRH ATPase cycle regulates the access of CK1a to phosphorylation sites in FRQ in cis, suggesting that FRH is an ATP-dependent remodelling factor acting on the protein complex. We show that the affinity of CK1a for FRQ decreases with increasing FRQ phosphorylation, suggesting functional inactivation of FRQ in the negative feedback loop of the circadian clock before and independent of its degradation.

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Section: Resultsmentioning

confidence: 99%

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confidence: 99%

The RNA helicase FRH is an ATP-dependent regulator of CK1a in the circadian clock of Neurospora crassa

et al. 2014

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“…Interestingly, this dual effect of ZTL on GI is reminiscent of the relationship between FREQUENCY (FRQ) and an RNA helicase (FRH) in the Neurospora clock. The formation of a FRQ-FRH complex (FCC) helps stabilize and retain FRQ in the cytosol, with increased FRQ nuclear levels when the interaction is disrupted or FRH levels are low (Cha et al, 2011). Conversely, the mammalian clock component mCRY helps retain the nucleocytoplasmic protein mPER2 in the nucleus and away from ubiquitylation and degradation in the cytosol (Yagita et al, 2002).…”

Section: Ztl-mediated Stabilization and Cytosolic Retention Of Gimentioning

confidence: 99%

The F-box protein ZEITLUPE controls stability and nucleocytoplasmic partitioning of GIGANTEA

et al. 2013

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SUMMARYNucleocytoplasmic partitioning of core clock components is essential for the proper operation of the circadian system. Previous work has shown that the F-box protein ZEITLUPE (ZTL) and clock element GIGANTEA (GI) heterodimerize in the cytosol, thereby stabilizing ZTL. Here, we report that ZTL post-translationally and reciprocally regulates protein levels and nucleocytoplasmic distribution of GI in Arabidopsis. We use ectopic expression of the N-terminus of ZTL, which contains the novel, light-absorbing region of ZTL (the LOV domain), transient expression assays and ztl mutants to establish that the levels of ZTL, a cytosolic protein, help govern the abundance and distribution of GI in the cytosol and nucleus. Ectopic expression of the ZTL N-terminus lengthens period, delays flowering time and alters hypocotyl length. We demonstrate that these phenotypes can be explained by the competitive interference of the LOV domain with endogenous GI-ZTL interactions. A complex of the ZTL N-terminus polypeptide with endogenous GI (LOV-GI) blocks normal GI function, causing degradation of endogenous ZTL and inhibition of other GI-related phenotypes. Increased cytosolic retention of GI by the LOV-GI complex additionally inhibits nuclear roles of GI, thereby lengthening flowering time. Hence, we conclude that under endogenous conditions, GI stabilization and cytoplasmic retention occurs naturally through a LOV domainmediated GI-ZTL interaction, and that ZTL indirectly regulates GI nuclear pools by sequestering GI to the cytosol. As the absence of either GI or ZTL compromises clock function and diminishes the protein abundance of the other, our results highlight how their reciprocal co-stabilization is essential for robust circadian oscillations.

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“…Despite the presence of the nuclear localization signal, most FRQ protein is cytoplasmic, suggesting that there is an active process to export FRQ from the nucleus. Using FRQ deletion mutants, the C-terminus of FRQ that includes the FRQ/FRQ-interacting RNA helicase (FRH) interaction domain was found to play an important role for cytoplasmic localization of FRQ (Cha et al ., 2011). Other domains in FRQ include a casein kinase I (CK1) interaction domain located in the middle of the protein (Guo et al ., 2010) and two PEST domains that function in FRQ turnover (Görl et al ., 2001).…”

Section: The Genetics and Biochemistry Of The Frq/wcc Feedback Loopmentioning

confidence: 99%

The Genetics of Circadian Rhythms in Neurospora

Lakin-Thomas¹,

Bell-Pedersen²,

Brody³

2011

The Genetics of Circadian Rhythms

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This chapter describes our current understanding of the genetics of the Neurospora clock and summarizes the important findings in this area in the past decade. Neurospora is the most intensively studied clock system, and the reasons for this are listed. A discussion of the genetic interactions between clock mutants is included, highlighting the utility of dissecting complex mechanisms by genetic means. The molecular details of the Neurospora circadian clock mechanism are described, as well as the mutations that affect the key clock proteins, FRQ, WC-1, and WC-2, with an emphasis on the roles of protein phosphorylation. Studies on additional genes affecting clock properties are described and place these genes into two categories: those that affect the FRQ/WCC oscillator and those that do not. A discussion of temperature compensation and the mutants affecting this property is included. A section is devoted to the observations pertinent to the existence of other oscillators in this organism with respect to their properties, their effects, and their preliminary characterization. The output of the clock and the control of clock-controlled genes are discussed, emphasizing the phasing of these genes and the layers of control. In conclusion, the authors provide an outlook summarizing their suggestions for areas that would be fruitful for further exploration.

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Regulation of the Activity and Cellular Localization of the Circadian Clock Protein FRQ

Cited by 44 publications

References 54 publications

The RNA helicase FRH is an ATP-dependent regulator of CK1a in the circadian clock of Neurospora crassa

The RNA helicase FRH is an ATP-dependent regulator of CK1a in the circadian clock of Neurospora crassa

The F-box protein ZEITLUPE controls stability and nucleocytoplasmic partitioning of GIGANTEA

The Genetics of Circadian Rhythms in Neurospora

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