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Human D-Amino Acid Oxidase: Structure, Function, and Regulation

TLDR
The known properties of human DAAO suggest that its activity must be finely tuned to fulfill a main physiological function such as the control of D-serine levels in the brain as well as the role of post-translational modifications on its main biochemical properties at the cellular level.
Abstract
D-Amino acid oxidase (DAAO) is an FAD-containing flavoenzyme that catalyzes with absolute stereoselectivity the oxidative deamination of all natural D-amino acids, the only exception being the acidic ones. This flavoenzyme plays different roles during evolution and in different tissues in humans. Its three-dimensional structure is well conserved during evolution: minute changes are responsible for the functional differences between enzymes from microorganism sources and those from humans. In recent years several investigations focused on human DAAO, mainly because of its role in degrading the neuromodulator D-serine in the central nervous system. D-Serine is the main coagonist of N-methyl D-aspartate receptors, i.e., excitatory amino acid receptors critically involved in main brain functions and pathologic conditions. Human DAAO possesses a weak interaction with the FAD cofactor; thus, in vivo it should be largely present in the inactive, apoprotein form. Binding of active-site ligands and the substrate stabilizes flavin binding, thus pushing the acquisition of catalytic competence. Interestingly, the kinetic efficiency of the enzyme on D-serine is very low. Human DAAO interacts with various proteins, in this way modulating its activity, targeting, and cell stability. The known properties of human DAAO suggest that its activity must be finely tuned to fulfill a main physiological function such as the control of D-serine levels in the brain. At present, studies are focusing on the epigenetic modulation of human DAAO expression and the role of post-translational modifications on its main biochemical properties at the cellular level.

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Journal ArticleDOI

L-serine synthesis via the phosphorylated pathway in humans

TL;DR: It is believed that an in-depth investigation of these enzymes is crucial to identify the molecular mechanisms involved in modulating concentrations of the serine enantiomers and for studying the interplay between glial and neuronal cells and also to determine the most suitable therapeutic approach for various diseases.
Journal ArticleDOI

D-cysteine is an endogenous regulator of neural progenitor cell dynamics in the mammalian brain.

TL;DR: Using chiral high-performance liquid chromatography and a stereospecific luciferase assay, this paper identified endogenous d-cysteine in the mammalian brain and implicate it as a physiologic regulator of NPC homeostasis in the developing brain.
Journal ArticleDOI

The Role of D-Amino Acids in Alzheimer's Disease.

TL;DR: In this paper, the experimental findings linking D-serine and D-aspartate, through NMDA receptor modulation, to AD and cognitive functions, were reported, which was also associated with the enzymes related to D-amino acid metabolism as well as with glucose and serine metabolism.
Journal ArticleDOI

The Role of Host-Generated H2S in Microbial Pathogenesis: New Perspectives on Tuberculosis.

TL;DR: The current understanding of the role of host-derived H2S in tuberculosis (TB) disease, including its influences on host immunity and bioenergetics, and on Mycobacterium tuberculosis (Mtb) growth and survival is described.
References
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Journal ArticleDOI

Identification of Novel d-Amino Acid Oxidase Inhibitors by in Silico Screening and Their Functional Characterization in Vitro

TL;DR: Results reported in this study indicate that some of these compounds are possible lead compounds for the development of a clinically useful DAO inhibitor and have the potential to serve as active site probes to elucidate the structure-function relationships of DAO.
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D-serine signalling as a prominent determinant of neuronal-glial dialogue in the healthy and diseased brain.

TL;DR: D‐serine regulation of synaptic transmission and plasticity and its role in normal aging and Alzheimer's disease and schizophrenia are studied.
Journal ArticleDOI

Optimization of human D-amino acid oxidase expression in Escherichia coli.

TL;DR: Optimization of medium ingredients, of the time and the amount of inducer's addition, pH control at the moment of induction and harvest, low mechanical shear stress regime during recombinant protein production, represent the factors concurring to achieve the reported expression level.
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Chlorpromazine oligomer is a potentially active substance that inhibits human D-amino acid oxidase, product of a susceptibility gene for schizophrenia.

TL;DR: The inhibitory effect of an antipsychotic drug, chlorpromazine, on humanDAO is shown, which is consistent with previous reports using porcine DAO, although human DAO was inhibited to a lesser degree than porcINE DAO.
Journal ArticleDOI

Mutual regulation between serine and nitric oxide metabolism in human glioblastoma cells.

TL;DR: Shoji et al. as discussed by the authors showed that D-serine indirectly caused dose-and time-dependent inhibition of neuronal nitric oxide synthase (nNOS) without affecting endothelial NOS in human glioblastoma cell line U87.
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