Restructuring of the dinucleotide-binding fold in an NADP(H) sensor protein

Zheng, Xiaofeng; Dai, Xueyu; Zhao, Yanmei; Chen, Qiang; Lu, Fei; Yao, Deqiang; Yu, Quan; Liu, Xinping; Zhang, Chuanmao; Gu, Xiaocheng; Luo, Ming

doi:10.1073/pnas.0700480104

Cited by 56 publications

(62 citation statements)

References 35 publications

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“…The human protein HSCARG (NmrA-like family domaincontaining protein 1 or NMRAL1) has been identified as a novel NADPH sensor Zheng et al, 2007). Our previous studies have shown that HSCARG restructures and redistributes in response to changes of intracellular NADPH/NADP + levels Zheng et al, 2007) and found that HSCARG is involved in the regulation of nitric oxide (NO) production through repression of the activity of argininosuccinate synthetase (AS), a rate-limiting enzyme in NO synthesis .…”

Section: Introductionmentioning

confidence: 99%

“…Our previous studies have shown that HSCARG restructures and redistributes in response to changes of intracellular NADPH/NADP + levels Zheng et al, 2007) and found that HSCARG is involved in the regulation of nitric oxide (NO) production through repression of the activity of argininosuccinate synthetase (AS), a rate-limiting enzyme in NO synthesis . The interaction between HSCARG and AS is enhanced when the intracellular NADPH/NADP + levels decreased and leads to a stronger inhibition by HSCARG on AS and NO production.…”

Section: Introductionmentioning

confidence: 99%

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HSCARG inhibits activation of NF-κB by interacting with IκB kinase-β

Gan

Lian

et al. 2009

Journal of Cell Science

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HSCARG is a recently identified human NADPH sensor. Our previous studies have shown that HSCARG can affect NO production and cell viability, but the signal pathway mediated by this protein is unknown. Here, we show that HSCARG is involved in the NF-B signaling pathway and find that HSCARG suppresses TNF-and IL1-induced NF-B activation in a dose-dependent manner. Co-immunoprecipitation and immunofluorescence analyses demonstrate that HSCARG interacts and colocalizes with IKK. HSCARG inhibits the phosphorylation of IKK and further blocks the degradation of IB, the substrate of IKK, which retains NF-B in the cytoplasm and suppresses its activity. In addition, our data indicate that IKK is required for HSCARG-inhibited NF-B activation. Our findings delineate a pathway by which HSCARG negatively regulates NF-B activation.Supplementary material available online at

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

HSCARG inhibits activation of NF-κB by interacting with IκB kinase-β

Gan

Lian

et al. 2009

Journal of Cell Science

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“…27 In this respect we note that the Human protein HSCARG, which belongs to the NmrA-like structural family, binds NADPH with a 360-fold lower K D than that for NADP þ . 15 Given these observations, a redox sensing role for NmrA is less likely.…”

Section: Discussionmentioning

confidence: 99%

“…13 HSCARG is essential for epithelial cell viability, binds NADPH much more strongly than NADP þ and may link changes in the NADP þ : NADPH ratio to modulation of the production of the important cell signaling molecule nitric oxide. [14][15][16] Microcalorimetry experiments showed that NmrA binds NAD þ and NADP þ with similar affinity but has a greatly reduced affinity for NADH and NADPH. The structure of NmrA in a complex with NADP þ has shown how repositioning a His 37 sidechain allows the different conformations of NAD þ and NADP þ to be accommodated.…”

Section: Introductionmentioning

confidence: 99%

The transcription repressor NmrA is subject to proteolysis by three Aspergillus nidulans proteases

et al. 2010

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The role of specific cleavage of transcription repressor proteins by proteases and how this may be related to the emerging theme of dinucleotides as cellular signaling molecules is poorly characterized. The transcription repressor NmrA of Aspergillus nidulans discriminates between oxidized and reduced dinucleotides, however, dinucleotide binding has no effect on its interaction with the zinc finger in the transcription activator AreA. Protease activity in A. nidulans was assayed using NmrA as the substrate, and was absent in mycelium grown under nitrogen sufficient conditions but abundant in mycelium starved of nitrogen. One of the proteases was purified and identified as the protein Q5BAR4 encoded by the gene AN2366.2. Fluorescence confocal microscopy showed that the nuclear levels of NmrA were reduced approximately 38% when mycelium was grown on nitrate compared to ammonium and absent when starved of nitrogen. Proteolysis of NmrA occurred in an ordered manner by preferential digestion within a C-terminal surface exposed loop and subsequent digestion at other sites. NmrA digested at the C-terminal site was unable to bind to the AreA zinc finger. These data reveal a potential new layer of control of nitrogen metabolite repression by the ordered proteolytic cleavage of NmrA. NmrA digested at the C-terminal site retained the ability to bind NAD 1 and showed a resistance to further digestion that was enhanced by the presence of NAD 1 . This is the first time that an effect of dinucleotide binding to NmrA has been demonstrated.

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“…It also shows close homology with UDP-galactose 4-epimerase. It is known that NmrA protein binds oxidized NAD which has probably certain regulating function (Zheng et al 2007). Its dehydrogenase and reductase activity probably does not work in this case ?…”

Section: Discussionmentioning

confidence: 99%