Quinone sensing by the circadian input kinase of the cyanobacterial circadian clock

Ivleva, Natalia B.; Gao, Tiyu; LiWang, Andy; Golden, Susan S.

doi:10.1073/pnas.0606639103

Cited by 108 publications

(156 citation statements)

References 47 publications

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“…Accumulation of CikA occurs during the night (Ivleva et al 2006), and low levels of CikA protein are present at higher light intensities. Levels of CikA protein are locked at the low level that is associated with high light in strains deficient in ldpA (Ivleva et al 2005).…”

Section: Inputmentioning

confidence: 99%

“…Both CikA and LdpA have been shown to be part of the Kai protein complex (along with the output protein SasA, discussed below), and at least CikA influences the phosphorylation state of KaiC (Ivleva et al 2005(Ivleva et al , 2006. The assembly and disassembly of this large heteromultimeric protein complex, termed the "periodosome," appear to be a driving force behind the cyanobacterial circadian system as a whole.…”

Section: Inputmentioning

confidence: 99%

“…Levels of CikA protein are locked at the low level that is associated with high light in strains deficient in ldpA (Ivleva et al 2005). Degradation of CikA can be stimulated by the direct binding of a quinone analog 2,5-dibromo-3-methyl-6-isopropyl-p-benzoquinone (DBMIB) to the pseudo-receiver domain of the protein (Ivleva et al 2006). DBMIB affects electron transport in the photosynthetic apparatus to produce an excess of electrons (reduction), which reflects the redox state of the cell.…”

Section: Inputmentioning

confidence: 99%

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Biological Rhythms Workshop IA: Molecular Basis of Rhythms Generation

Mackey¹

2007

Cold Spring Harbor Symposia on Quantitative Biology

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Current circadian models are based on genetic, biochemical, and structural data that, when combined, provide a comprehensive picture of the molecular basis for rhythms generation. These models describe three basic elements-input pathways, oscillator, and output pathways-to which each molecular component is assigned. The lines between these elements are often blurred because some proteins function in more than one element of the circadian system. The end result of these molecular oscillations is the same in each system (near 24-hour timing), yet the proteins involved, the interactions among those proteins, and the regulatory feedback loops differ. Here, the current models for the molecular basis for rhythms generation are described for the prokaryotic cyanobacterium Synechococcus elongatus as well as the eukaryotic systems Neurospora crassa, Drosophila melanogaster, Arabidopsis thaliana, and mammals (particularly rodents).

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Section: Inputmentioning

confidence: 99%

Section: Inputmentioning

confidence: 99%

Section: Inputmentioning

confidence: 99%

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Biological Rhythms Workshop IA: Molecular Basis of Rhythms Generation

Mackey¹

2007

Cold Spring Harbor Symposia on Quantitative Biology

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“…The regulation of transcription is not the only mechanism that controls clock progression, as modulation of protein stability has emerged as an important aspect of the circadian clockwork (Millar, 2000;Harms et al, 2004;Shu and Hong-Hui, 2004;Liu, 2005;Ivleva et al, 2006;Dardente and Cermakian, 2007;Farre and Kay, 2007;Gallego and Virshup, 2007). ZEITLUPE (ZTL), the founding member of the protein family characterized by a LIGHT, OXYGEN, or VOLTAGE (LOV) domain, an F-box motif, and kelch repeats, mediates the degradation of TOC1 via the formation of a multiprotein Skp/Cullin1/F-box complex that catalyzes the ubiquitylation of proteins destined for proteasomal degradation (Kiyosue and Wada, 2000;Somers et al, 2000Somers et al, , 2004Schultz et al, 2001;Han et al, 2004;Fukamatsu et al, 2005;Kevei et al, 2006).…”

Section: Introductionmentioning

confidence: 99%

PRR3 Is a Vascular Regulator of TOC1 Stability in theArabidopsisCircadian Clock

et al. 2007

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The pseudoresponse regulators (PRRs) participate in the progression of the circadian clock in Arabidopsis thaliana. The founding member of the family, TIMING OF CAB EXPRESSION1 (TOC1), is an essential component of the transcriptional network that constitutes the core mechanism of the circadian oscillator. Recent data suggest a role in circadian regulation for all five members of the PRR family; however, the molecular function of TOC1 or any other PRRs remains unknown. In this work, we present evidence for the involvement of PRR3 in the regulation of TOC1 protein stability. PRR3 was temporally coexpressed with TOC1 under different photoperiods, yet its tissue expression was only partially overlapping with that of TOC1, as PRR3 appeared restricted to the vasculature. Decreased expression of PRR3 resulted in reduced levels of TOC1 protein, while overexpression of PRR3 caused an increase in the levels of TOC1, all without affecting the amount of TOC1 transcript. PRR3 was able to bind to TOC1 in yeast and in plants and to perturb TOC1 interaction with ZEITLUPE (ZTL), which targets TOC1 for proteasome-dependent degradation. Together, our results indicate that PRR3 might function to modulate TOC1 stability by hindering ZTL-dependent TOC1 degradation, suggesting the existence of local regulators of clock activity and adding to the growing importance of posttranslational regulation in the design of circadian timing mechanisms in plants.

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“…We believe that this chromophore is bacteriochlorophyll bound by the LH peptides, which absorbs light and transmits it to the reaction center, where it is used to reduce quinones in the membrane. In other systems, the redox status of the quinone pool changes under different light intensities, and light intensity is sensed as a change in the redox state of the quinone pool (35)(36)(37)(38)(39)(40). We hypothesize that light intensity is sensed as a redox signal by R. palustris, and that this redox signal combined with the pool of active BphPs (even in the absence of BV) is sufficient for LH4 synthesis.…”

Section: Discussionmentioning

confidence: 99%

Apo-bacteriophytochromes modulate bacterial photosynthesis in response to low light

Fixen

Baker

Stojković

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

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Significance Bacteriophytochromes (BphPs) are regulatory proteins that bind a light-absorbing chromophore called biliverdin. Recombinant BphPs show promise for use in regulating neuron function in mammals with light. We explored the possibility that BphPs may sense cues in addition to light. Our motivation was that biliverdin requires oxygen for its synthesis, and some bacteria use BphPs to control photosynthesis in the absence of oxygen. We found that the photosynthetic bacterium Rhodopseudomonas palustris requires two BphP proteins to sense low light when grown in the absence of oxygen; however, the BphPs do not need to have their chromophore to sense low light intensities. BphPs may respond to intracellular signals, such as reducing conditions, in addition to light to regulate downstream functions.

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Quinone sensing by the circadian input kinase of the cyanobacterial circadian clock

Cited by 108 publications

References 47 publications

Biological Rhythms Workshop IA: Molecular Basis of Rhythms Generation

Biological Rhythms Workshop IA: Molecular Basis of Rhythms Generation

PRR3 Is a Vascular Regulator of TOC1 Stability in theArabidopsisCircadian Clock

Apo-bacteriophytochromes modulate bacterial photosynthesis in response to low light

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