Citrulline‐nitric oxide cycle protein‐protein interactions

Renal function is highly dependent on endothelium-derived nitric oxide (NO). Several renal disorders have been linked to impaired NO bioavailability. The enzyme that is responsible for the synthesis of NO within the renal endothelium is endothelial NO synthase (eNOS). eNOS-mediated NO generation is a highly regulated cellular event, which is induced by calcium-mobilizing agonists and fluid shear stress. eNOS activity is regulated at the transcriptional level but also by a variety of modifications, such as acylation and phosphorylation, by its cellular localization, and by protein-protein interactions. The present review focuses on the complex regulation of eNOS within the endothelial cell.

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Disrupting protein-protein interactions of neuronal nitric oxide synthase: implications in schizophrenia-related behaviours

European Neuropsychopharmacology ◽

10.1016/s0924-977x(17)31585-7 ◽

2017 ◽

Vol 27 ◽

pp. S887-S888

Author(s):

E. Candemir ◽

N. Fattakhov ◽

V. Frerichs ◽

S. Arshad ◽

A. O’Leary ◽

...

Keyword(s):

Nitric Oxide ◽

Nitric Oxide Synthase ◽

Protein Interactions ◽

Neuronal Nitric Oxide Synthase ◽

Protein Protein Interactions ◽

Oxide Synthase

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Protein interactions with nitric oxide synthases: controlling the right time, the right place, and the right amount of nitric oxide

AJP Renal Physiology ◽

10.1152/ajprenal.00048.2003 ◽

2003 ◽

Vol 285 (2) ◽

pp. F178-F190 ◽

Cited By ~ 179

Author(s):

Bruce C. Kone ◽

Teresa Kuncewicz ◽

Wenzheng Zhang ◽

Zhi-Yuan Yu

Keyword(s):

Nitric Oxide ◽

Protein Interactions ◽

Biological Effects ◽

Pdz Domain ◽

Membrane Receptors ◽

Heterologous Proteins ◽

Protein Protein Interactions ◽

Potential Implication ◽

The Right ◽

Nos Isoforms

Nitric oxide (NO) is a potent cell-signaling, effector, and vasodilator molecule that plays important roles in diverse biological effects in the kidney, vasculature, and many other tissues. Because of its high biological reactivity and diffusibility, multiple tiers of regulation, ranging from transcriptional to posttranslational controls, tightly control NO biosynthesis. Interactions of each of the major NO synthase (NOS) isoforms with heterologous proteins have emerged as a mechanism by which the activity, spatial distribution, and proximity of the NOS isoforms to regulatory proteins and intended targets are governed. Dimerization of the NOS isozymes, required for their activity, exhibits distinguishing features among these proteins and may serve as a regulated process and target for therapeutic intervention. An increasingly wide array of proteins, ranging from scaffolding proteins to membrane receptors, has been shown to function as NOS-binding partners. Neuronal NOS interacts via its PDZ domain with several PDZ-domain proteins. Several resident and recruited proteins of plasmalemmal caveolae, including caveolins, anchoring proteins, G protein-coupled receptors, kinases, and molecular chaperones, modulate the activity and trafficking of endothelial NOS in the endothelium. Inducible NOS (iNOS) interacts with the inhibitory molecules kalirin and NOS-associated protein 110 kDa, as well as activator proteins, the Rac GTPases. In addition, protein-protein interactions of proteins governing iNOS transcription function to specify activation or suppression of iNOS induction by cytokines. The calpain and ubiquitin-proteasome pathways are the major proteolytic systems responsible for the regulated degradation of NOS isozymes. The experimental basis for these protein-protein interactions, their functional importance, and potential implication for renal and vascular physiology and pathophysiology is reviewed.

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Compensatory Phosphorylation and Protein-Protein Interactions Revealed by Loss of Function and Gain of Function Mutants of Multiple Serine Phosphorylation Sites in Endothelial Nitric-oxide Synthase

Journal of Biological Chemistry ◽

10.1074/jbc.m211926200 ◽

2003 ◽

Vol 278 (17) ◽

pp. 14841-14849 ◽

Cited By ~ 169

Author(s):

Philip M. Bauer ◽

David Fulton ◽

Yong Chool Boo ◽

George P. Sorescu ◽

Bruce E. Kemp ◽

...

Keyword(s):

Nitric Oxide ◽

Nitric Oxide Synthase ◽

Protein Interactions ◽

Endothelial Nitric Oxide Synthase ◽

Serine Phosphorylation ◽

Phosphorylation Sites ◽

Loss Of Function ◽

Protein Protein Interactions ◽

Oxide Synthase ◽

Endothelial Nitric Oxide

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Sulfur: the heart of nitric oxide-dependent redox signalling

Journal of Experimental Botany ◽

10.1093/jxb/erz135 ◽

2019 ◽

Vol 70 (16) ◽

pp. 4279-4286 ◽

Cited By ~ 6

Author(s):

Saima Umbreen ◽

Jibril Lubega ◽

Gary J Loake

Keyword(s):

Nitric Oxide ◽

Protein Interactions ◽

Protein Function ◽

Protein Protein Interactions ◽

Post Translational Modification ◽

Redox Signalling ◽

Signalling Molecule ◽

Environmental Relations ◽

Plant Pathogen Interactions ◽

Modify Protein

Abstract Nitric oxide (NO), more benign than its more reactive and damaging related molecules, reactive oxygen species (ROS), is perfectly suited for duties as a redox signalling molecule. A key route for NO bioactivity is through S-nitrosation, the addition of an NO moiety to a protein Cys thiol (-SH). This redox-based, post-translational modification (PTM) can modify protein function analogous to more well established PTMs such as phosphorylation, for example by modulating enzyme activity, localization, or protein–protein interactions. At the heart of the underpinning chemistry associated with this PTM is sulfur. The emerging evidence suggests that S-nitrosation is integral to a myriad of plant biological processes embedded in both development and environmental relations. However, a role for S-nitrosation is perhaps most well established in plant–pathogen interactions.

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Pharmacologic Manipulation of Nitric Oxide Signaling: Targeting NOS Dimerization and Protein-Protein Interactions

Current Topics in Medicinal Chemistry ◽

10.2174/156802607779318253 ◽

2007 ◽

Vol 7 (1) ◽

pp. 97-114 ◽

Cited By ~ 35

Author(s):

Jeremy Paige ◽

Samie Jaffrey

Keyword(s):

Nitric Oxide ◽

Protein Interactions ◽

Protein Protein Interactions ◽

Nitric Oxide Signaling

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Characterization of endothelial argininosuccinate synthase subcellular localization and protein interactions relevant to the function of the citrulline‐nitric oxide cycle

The FASEB Journal ◽

10.1096/fasebj.23.1_supplement.852.1 ◽

2009 ◽

Vol 23 (S1) ◽

Author(s):

Karen Davidowitz Corbin ◽

Laura C Pendleton ◽

Sandra K Shriver ◽

Duane C Eichler

Keyword(s):

Nitric Oxide ◽

Subcellular Localization ◽

Protein Interactions ◽

Argininosuccinate Synthase ◽

Nitric Oxide Cycle

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Neonatal Isoflurane Anesthesia or Disruption of Postsynaptic Density-95 Protein Interactions Change Dendritic Spine Densities and Cognitive Function in Juvenile Mice

Anesthesiology ◽

10.1097/aln.0000000000003482 ◽

2020 ◽

Vol 133 (4) ◽

pp. 812-823

Author(s):

Michele L. Schaefer ◽

Patric J. Perez ◽

Meina Wang ◽

Christy Gray ◽

Caroline Krall ◽

...

Keyword(s):

Nitric Oxide ◽

Protein Interactions ◽

Postsynaptic Density ◽

Long Term Potentiation ◽

Fear Learning ◽

Nitric Oxide Donor ◽

Spine Density ◽

Protein Protein Interactions ◽

Term Potentiation

Background Experimental evidence shows postnatal exposure to anesthesia negatively affects brain development. The PDZ2 domain, mediating protein–protein interactions of the postsynaptic density-95 protein, serves as a molecular target for several inhaled anesthetics. The authors hypothesized that early postnatal disruption of postsynaptic density-95 PDZ2 domain interactions has persistent effects on dendritic spines and cognitive function. Methods One-week-old mice were exposed to 1.5% isoflurane for 4 h or injected with 8 mg/kg active postsynaptic density-95 wild-type PDZ2 peptide along with their respective controls. A subset of these mice also received 4 mg/kg of the nitric oxide donor molsidomine. Hippocampal spine density, long-term potentiation, novel object recognition memory, and fear learning and memory were evaluated in mice. Results Exposure of 7-day-old mice to isoflurane or postsynaptic density-95 wild-type PDZ2 peptide relative to controls causes: (1) a long-term decrease in mushroom spines at 7 weeks (mean ± SD [spines per micrometer]): control (0.8 ± 0.2) versus isoflurane (0.4 ± 0.2), P < 0.0001, and PDZ2MUT (0.7 ± 0.2) versus PDZ2WT (0.4 ± 0.2), P < 0.001; (2) deficits in object recognition at 6 weeks (mean ± SD [recognition index]): naïve (70 ± 8) versus isoflurane (55 ± 14), P = 0.010, and control (65 ± 13) versus isoflurane (55 ± 14), P = 0.045, and PDZ2MUT (64 ±11) versus PDZ2WT (53 ± 18), P = 0.045; and (3) deficits in fear learning at 7 weeks and memory at 8 weeks (mean ± SD [% freezing duration]): Learning, control (69 ± 12) versus isoflurane (52 ± 13), P < 0.0001, and PDZ2MUT (65 ± 14) versus PDZ2WT (55 ± 14) P = 0.011, and Memory, control (80 ± 17) versus isoflurane (56 ± 23), P < 0.0001 and PDZ2MUT (73 ± 18) versus PDZ2WT (44 ± 19) P < 0.0001. Impairment in long-term potentiation has fully recovered here at 7 weeks (mean ± SD [% baseline]): control (140 ± 3) versus isoflurane (137 ± 8), P = 0.560, and PDZ2MUT (136 ± 17) versus PDZ2WT (128 ± 11), P = 0.512. The isoflurane induced decrease in mushroom spines was preventable by introduction of a nitric oxide donor. Conclusions Early disruption of PDZ2 domain-mediated protein–protein interactions mimics isoflurane in decreasing mushroom spine density and causing learning and memory deficits in mice. Prevention of the decrease in mushroom spine density with a nitric oxide donor supports a role for neuronal nitric oxide synthase pathway in mediating this cellular change associated with cognitive impairment. Editor’s Perspective What We Already Know about This Topic What This Article Tells Us That Is New

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