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The Antidepressant/Antipanic/Neuroprotective Drug Phenelzine: Neuropharmacological and Drug Metabolism StudiesKumpula, David J Unknown Date
No description available.
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Le Bisphénol A dans la prééclampsie / Bisphenol A in preeclampsiaChapdelaine, Alexandra January 2016 (has links)
Résumé : La prééclampsie (PE) est un désordre de la grossesse caractérisée par une dysfonction endothéliale faisant en sorte que l’endothélium devient moins sensible aux signaux de vasodilatation. La réponse provoquée par la liaison de la sérotonine au sous-type de récepteur S[indice inférieur 2] entraîne la libération de molécules aux propriétés vasoconstrictrices, qui, par une boucle de rétroaction positive, entraîne la libération de davantage de sérotonine par les plaquettes. Cette boucle amplifie la réponse et contribue ainsi à l’hypertension présente chez les femmes ayant une PE. Précédemment, il a été démontré par notre laboratoire que le Bisphénol A (BPA) s’accumulait davantage dans le placenta des femmes avec PE en comparaison aux femmes normotensives. Cette accumulation pourrait découler d’une perturbation de sa métabolisation qui impliquerait notamment la β-glucuronidase (GUSB). Des études chez les animaux ont quant à elles démontré que le BPA pouvait inhiber l’activité de la monoamine oxydase (MAO) à forte dose. Nous avons étudié l’effet du BPA à faible concentration (10 ng/ml) sur la MAO-A des cellules placentaires et démontré que le BPA inhibait la MAO-A de façon significative sans affecter son expression protéique. Afin d’expliquer l’accumulation particulière du BPA chez les femmes PE, nous avons comparé l’activité spécifique et l’expression protéique de la β-glucuronidase (GUSB) placentaire en utilisant un devis cas-témoins. Une tendance non significative suggère que la GUSB pourrait partiellement contribuer à l’accumulation du BPA chez les femmes PE. Nous avons étudié la relation entre la concentration sérique maternelle de BPA et la concentration à laquelle le fœtus est exposé par régression linéaire et corrélation de Spearman. Un tel modèle ne pourrait être utilisé pour déterminer de façon quantitative l’exposition fœtale. En revanche, en vue de la forte corrélation entre ces deux variables, une haute concentration sérique maternelle de BPA devrait se refléter par une haute exposition fœtale. Cette corrélation implique aussi que le métabolisme placentaire ne joue pas un rôle significatif dans la protection du fœtus. Le BPA pourrait ainsi contribuer à l’hypertension chez les femmes PE présentant une dysfonction endothéliale en inhibant la MAO-A et ainsi, favorisant la hausse de sérotonine circulante. Cette étude suggère les bases d’un mécanisme par lequel le BPA s’accumulerait davantage chez les femmes PE et affecterait ainsi la MAO-A placentaire et potentiellement, la MAO-A fœtale vu ses propriétés physico-chimiques. / Abstract : Preeclampsia (PE) is an hypertensive disorder of pregnancy characterized by a generalized endothelial dysfunction where the response to vasodilatation signals is compromised. The binding of serotonin to its S[subscript 2] receptor subtype 2 releases vasoconstrictor molecules which, by a positive retroaction loop, stimulates the release of more serotonin from platelets. This positive retroaction loop stimulates the vasoconstriction of blood vessels and contributes to the hypertension in women with PE. Previously, we showed that Bisphenol A (BPA) accumulates more in the placenta of women with PE than in normotensive women. This accumulation may be the result of an impaired metabolization due to the action of the β-Glucuronidase (GUSB). Animal studies showed that BPA at high dose could lower the activity of the monoamine oxidase A (MAO-A), an enzyme implicated in the metabolism of serotonin. We studied the impact of BPA at low dose (10 ng/ml) in trophoblastic primary cells and showed that even at low dose, BPA can lower its activity without affecting the protein expression. To determine if GUSB could be the cause of the BPA accumulation in women with PE, we studied its activity and protein expression in placental biopsies from women with and without PE. A nonsignificant tendency showed that the GUSB activity and protein expression were higher in women with PE. To study the impact of placental metabolism in the fetal exposure, we studied the relation between maternal and fetal concentrations of BPA with linear regression analysis and Spearman’s correlation. We showed that maternal BPA could not precisely predict the fetal exposure and that the placental metabolism is probably limited in light of the strong correlation between both variables. This strong correlation also implied that high maternal exposure would result in high fetal exposure. This study shows that the accumulation of BPA in preeclamptic women could contribute to maternal hypertension by interacting with serotonin levels. This accumulation could partially be attributed to a higher GUSB, but other factors are probably implicated. The strong correlation between maternal and fetal exposure implies that the placental metabolism of BPA is limited and does not protect the fetus significantly. This study suggests the basis of a mechanism explaining the abnormal accumulation of BPA in the placenta in women with PE and its impact on the placental MAO-A and potentially, the foetal MAO-A because of its physico-chemical properties.
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Biochemical aspects of monoamine oxidase in rat brain and liver.January 1980 (has links)
by Kwok-Ping Ho. / Thesis (M.Phil.)--Chinese University of Hong Kong, 1980. / Bibliography: leaves 111-118.
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Screening of virtual libraries for monoamine oxidase inhibitors / Melinda BarkhuizenBarkhuizen, Melinda January 2013 (has links)
The traditional view of drug design is that a single drug should interact with a single
molecular target. As science progressed, there was an understanding that most drugs
interact with more than one target and that multiple targets may be responsible for either
adverse effects or additional therapeutic effects. The idea of polypharmacology, which
suggests that the focus of drug design should shift from a single drug that interacts with a
single target to a single drug that can have interactions with multiple targets and multiple
therapeutic effects, revolutionized the drug discovery process. Discovering new drugs is a
long and costly process with years of research and development and clinical trials required
before the drugs reach the market for much needed therapeutic applications. By repurposing
drugs that are already on the market for a new therapeutic target, the discovery process is
accelerated significantly.
One such a target disease, for which there is a great need for new effective therapies, is
Parkinson’s disease (PD). PD is a progressive neurodegenerative disease that is caused by
the death of dopaminergic neurons in the substantia nigra with the resulting loss of
dopamine from the striatum. Degeneration in PD leads to varying degrees of motor difficulty
and disability, along with other symptoms. Current therapies are focussed on symptomatic
management and an improvement of the quality of life of patients, rather than on a cure.
There are several therapeutic targets that are currently used in the treatment of PD. One of
those targets is the monoamine oxidase (MAO) enzymes, in particular the MAO-B isoform.
The MAO enzymes are responsible for the metabolism of amine neurotransmitters, such as
dopamine, and inhibition of MAO-B has proven to be an effective strategy to increase the
dopamine levels in the brain. Clinically, selective MAO-B inhibitors are administered
concurrently with levodopa (a precursor of dopamine) to increase the levels of dopamine
derived from levodopa. This approach prolongs the beneficial effects of levodopa.
Because MAO-A is responsible for the breakdown of noradrenalin, adrenalin, serotonin and
tyramine, non-selective and selective MAO-A inhibitors have therapeutic applications in
other neurological and psychiatric disorders such as depression. MAO-A inhibitors,
particularly irreversible inhibitors, are also notable from a toxicological point of view.
Irreversible MAO-A inhibitors may lead to potentially dangerous effects when combined with
serotonergic drugs and certain foods containing tyramine, such as cheeses and processed
meats. Selective MAO-B inhibitors and reversible MAO-A inhibitors appear to be free of
these interactions. Based on the considerations above, this study aimed to identify clinically used drugs which
also inhibit the MAO enzymes as a secondary pharmacological property. Such drugs may, in
theory, be repurposed as MAO inhibitors for therapeutic use in the treatment of PD and
depression. The identification of potential MAO-A inhibitory properties among clinically used
drugs are of further importance since the irreversible inhibition of MAO-A may lead to
dangerous effects when combined with certain drugs and foods.
To screen clinically used drugs for potential MAO-A and MAO-B inhibitory activities, a
pharmacophore approach was followed. A pharmacophore model is a virtual 3D
representation of the common steric and electrostatic features of the interaction between an
enzyme and a ligand. By identifying hydrogen bond acceptor, hydrogen bond donor and
hydrophobic interactions between a reference ligand and an enzyme, a model is created that
can search databases for other molecules that would have similar interactions with the
enzyme and arguably also act as ligands. This enables the screening of a large amount of
molecules in a short amount of time. To assist in the identification of MAO inhibitors,
pharmacophore models of the MAO enzymes were constructed using the known
crystallographic structures of MAO-A co-crystallized with harmine, and MAO-B cocrystallized
with safinamide. The Discovery Studio® software package (Accelrys) was used
for this purpose.
In this study, virtual libraries of United States Food and Drug Administration (FDA) approved
drugs and the United States Environmental Protection Agency (EPA) maximum daily dose
databases were screened with pharmacophore models of MAO-A and MAO-B. Among the
hits, 26 drugs were selected on the basis of availability and cost, and were subjected to in
vitro bio-assays in order to determine their potencies (IC50 values) as inhibitors of
recombinant human MAO-A and/or MAO-B. Among the drugs tested, 6 compounds
exhibited inhibitory activity towards the MAO enzymes. Of the 6 compounds, pentamidine
(IC50 = 0.61 μM for MAO-A and IC50 = 0.22 μM for MAO-B) and phenformin (IC50 = 41 μM for
MAO-A) were selected for further analysis.
An examination of the recoveries of the enzymatic activities after dilution and dialysis of the
enzyme-inhibitor complexes showed that both pentamidine and phenformin interact
reversibly with the MAO enzymes. A kinetic analysis suggests that pentamidine acts as a
competitive inhibitor with estimated Ki values of 0.41 μM and 0.22 μM for the inhibition of
MAO-A and MAO-B, respectively. An analysis of the available pharmacokinetic data and
typical therapeutic doses of phenformin and pentamidine suggests that the MAO inhibitory
potencies (and reversible mode of action) of phenformin are unlikely to be of
pharmacological relevance in humans. Pentamidine, on the other hand, is expected to interact with both MAO-A and MAO-B at typical therapeutic doses. Because of its MAO-A
inhibitory activity, pentamidine may thus, in theory, lead to a tyramine-associated
hypertensive crisis when combined with tyramine-containing foods. However, pentamidine is
unlikely to inhibit central MAO since it does not appear to penetrate the central nervous
system to a large degree.
In an attempt to gain further insight into the mode of binding to MAO, pentamidine and
phenformin were docked into models of the active sites of MAO-A and/or MAO-B. An
analysis of the interactions between the enzyme models and the ligands were carried out
and the results are discussed in the dissertation.
The results of this study show that the pharmacophore model approach may be useful in
identifying existing drugs with potential MAO inhibitory effects. The search for new
therapeutic MAO inhibitors, that can be used in the treatment of certain neurological
disorders, including PD and depression, may be accelerated by employing a virtual
screening approach. Such an approach may also be more cost effective than the de novo
design of MAO inhibitors. / MSc (Pharmaceutical Chemistry), North-West University, Potchefstroom Campus, 2014
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Screening of virtual libraries for monoamine oxidase inhibitors / Melinda BarkhuizenBarkhuizen, Melinda January 2013 (has links)
The traditional view of drug design is that a single drug should interact with a single
molecular target. As science progressed, there was an understanding that most drugs
interact with more than one target and that multiple targets may be responsible for either
adverse effects or additional therapeutic effects. The idea of polypharmacology, which
suggests that the focus of drug design should shift from a single drug that interacts with a
single target to a single drug that can have interactions with multiple targets and multiple
therapeutic effects, revolutionized the drug discovery process. Discovering new drugs is a
long and costly process with years of research and development and clinical trials required
before the drugs reach the market for much needed therapeutic applications. By repurposing
drugs that are already on the market for a new therapeutic target, the discovery process is
accelerated significantly.
One such a target disease, for which there is a great need for new effective therapies, is
Parkinson’s disease (PD). PD is a progressive neurodegenerative disease that is caused by
the death of dopaminergic neurons in the substantia nigra with the resulting loss of
dopamine from the striatum. Degeneration in PD leads to varying degrees of motor difficulty
and disability, along with other symptoms. Current therapies are focussed on symptomatic
management and an improvement of the quality of life of patients, rather than on a cure.
There are several therapeutic targets that are currently used in the treatment of PD. One of
those targets is the monoamine oxidase (MAO) enzymes, in particular the MAO-B isoform.
The MAO enzymes are responsible for the metabolism of amine neurotransmitters, such as
dopamine, and inhibition of MAO-B has proven to be an effective strategy to increase the
dopamine levels in the brain. Clinically, selective MAO-B inhibitors are administered
concurrently with levodopa (a precursor of dopamine) to increase the levels of dopamine
derived from levodopa. This approach prolongs the beneficial effects of levodopa.
Because MAO-A is responsible for the breakdown of noradrenalin, adrenalin, serotonin and
tyramine, non-selective and selective MAO-A inhibitors have therapeutic applications in
other neurological and psychiatric disorders such as depression. MAO-A inhibitors,
particularly irreversible inhibitors, are also notable from a toxicological point of view.
Irreversible MAO-A inhibitors may lead to potentially dangerous effects when combined with
serotonergic drugs and certain foods containing tyramine, such as cheeses and processed
meats. Selective MAO-B inhibitors and reversible MAO-A inhibitors appear to be free of
these interactions. Based on the considerations above, this study aimed to identify clinically used drugs which
also inhibit the MAO enzymes as a secondary pharmacological property. Such drugs may, in
theory, be repurposed as MAO inhibitors for therapeutic use in the treatment of PD and
depression. The identification of potential MAO-A inhibitory properties among clinically used
drugs are of further importance since the irreversible inhibition of MAO-A may lead to
dangerous effects when combined with certain drugs and foods.
To screen clinically used drugs for potential MAO-A and MAO-B inhibitory activities, a
pharmacophore approach was followed. A pharmacophore model is a virtual 3D
representation of the common steric and electrostatic features of the interaction between an
enzyme and a ligand. By identifying hydrogen bond acceptor, hydrogen bond donor and
hydrophobic interactions between a reference ligand and an enzyme, a model is created that
can search databases for other molecules that would have similar interactions with the
enzyme and arguably also act as ligands. This enables the screening of a large amount of
molecules in a short amount of time. To assist in the identification of MAO inhibitors,
pharmacophore models of the MAO enzymes were constructed using the known
crystallographic structures of MAO-A co-crystallized with harmine, and MAO-B cocrystallized
with safinamide. The Discovery Studio® software package (Accelrys) was used
for this purpose.
In this study, virtual libraries of United States Food and Drug Administration (FDA) approved
drugs and the United States Environmental Protection Agency (EPA) maximum daily dose
databases were screened with pharmacophore models of MAO-A and MAO-B. Among the
hits, 26 drugs were selected on the basis of availability and cost, and were subjected to in
vitro bio-assays in order to determine their potencies (IC50 values) as inhibitors of
recombinant human MAO-A and/or MAO-B. Among the drugs tested, 6 compounds
exhibited inhibitory activity towards the MAO enzymes. Of the 6 compounds, pentamidine
(IC50 = 0.61 μM for MAO-A and IC50 = 0.22 μM for MAO-B) and phenformin (IC50 = 41 μM for
MAO-A) were selected for further analysis.
An examination of the recoveries of the enzymatic activities after dilution and dialysis of the
enzyme-inhibitor complexes showed that both pentamidine and phenformin interact
reversibly with the MAO enzymes. A kinetic analysis suggests that pentamidine acts as a
competitive inhibitor with estimated Ki values of 0.41 μM and 0.22 μM for the inhibition of
MAO-A and MAO-B, respectively. An analysis of the available pharmacokinetic data and
typical therapeutic doses of phenformin and pentamidine suggests that the MAO inhibitory
potencies (and reversible mode of action) of phenformin are unlikely to be of
pharmacological relevance in humans. Pentamidine, on the other hand, is expected to interact with both MAO-A and MAO-B at typical therapeutic doses. Because of its MAO-A
inhibitory activity, pentamidine may thus, in theory, lead to a tyramine-associated
hypertensive crisis when combined with tyramine-containing foods. However, pentamidine is
unlikely to inhibit central MAO since it does not appear to penetrate the central nervous
system to a large degree.
In an attempt to gain further insight into the mode of binding to MAO, pentamidine and
phenformin were docked into models of the active sites of MAO-A and/or MAO-B. An
analysis of the interactions between the enzyme models and the ligands were carried out
and the results are discussed in the dissertation.
The results of this study show that the pharmacophore model approach may be useful in
identifying existing drugs with potential MAO inhibitory effects. The search for new
therapeutic MAO inhibitors, that can be used in the treatment of certain neurological
disorders, including PD and depression, may be accelerated by employing a virtual
screening approach. Such an approach may also be more cost effective than the de novo
design of MAO inhibitors. / MSc (Pharmaceutical Chemistry), North-West University, Potchefstroom Campus, 2014
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Molecular biology of X-chromosome diseaseChen, Zheng-Yi January 1992 (has links)
Genomic clones were isolated and characterized using the human monoamine oxidase A (MAOA) cDNA to screen a phage library, constructed from a human 4X cell line (48, XXXX). The genomic contig derived from overlapping phage clones showed that the size of the MAOA gene is over 80 kb. Exon-containing fragments from these phage clones were subcloned and sequenced. The data from this showed that the MAOA gene consists of 15 exons. A YAC (yeast artificial chromosome) isolated using the MAOA cDNA was characterized. This YAC was found to contain both the MAOA and the MAOB genes. Using PFGE (pulsed-field gel electrophoresis) to investigate the YAC, it was found that the MAOA and the MAOB genes are located within 50 kb and adjacent to each other. The two genes are localized in a 3'-to-3' fashion, suggesting their expression may be regulated independently. The analysis of the homology shown by the two genes clearly demonstrated that they were derived from duplication of a common ancestral gene. A CpG island was discovered to be associated with the 5' end of both genes. A restriction map of -2.5 Mb of genomic DMA around the MAO genes was generated by PFGE. Long-range mapping defined the physical relationship between the marker L1.28 and the MAO genes as L1.28_MAOA_MAOB. A number of genetic diseases have been linked to the Xp11.3 region. Strong linkage was known to exist between the Norrie disease locus and L1.28. Studies showed that some of the Norrie patients have deletions encompassing the region which contains L1.28 as well as the MAO genes. Another YAC isolated by using L1.28 as the probe was also characterized. A phage library was constructed from the L1.28 YAC and the end clones were isolated. Studies on some of the Norrie deletion patients showed that the proximal end clone of the YAC was retained in one of the deletion patients. Previous studies had shown that the Norrie disease locus was also localized proximal to the 5' end of the MAOB gene. The combined information placed the disease locus to an interval of 240 kb within the YAC. More phage clones were characterized in order to define further the region for the Norrie locus which was finally localized within 160 kb. A YAC fragment of 160 kb was isolated and used to screen two human retinal cDNA libraries. Among the cDNAs isolated, one group was found to be deleted in some of the Norrie patients previously without any known deletion, which established their candidacy as the transcripts of the Norrie disease locus. Further characterization of the candidate gene showed that it is conserved across species. The expression of the gene was detected in various tissues. The homology shared between the NDP gene and some of the growth factor binding proteins suggests its role in neural cell proliferation and differentiation.
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İntihar girişiminde bulunanlar arasında TP, 5-HTT, MAOA genlerinin polimorfizminin etkileri: gen-çevre etkileşiminin incelenmesi /Altınyazar, Vesile. Eren, İbrahim. January 2006 (has links) (PDF)
Tez (Tıpta Uzmanlık) - Süleyman Demirel Üniversitesi, Tıp Fakültesi, Ruh Sağlığı ve Hastalıkları Anabilim Dalı, 2006. / Bibliyografya var.
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Genetic studies of depressive symptoms/Jansson, Mårten, January 2004 (has links)
Diss. (sammanfattning) Stockholm : Karol. inst., 2004. / Härtill 4 uppsatser.
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Monoamine oxidase in relation to thyroid hormonesZile, Maija Helene, January 1959 (has links)
Thesis (Ph. D.)--University of Wisconsin--Madison, 1959. / Typescript. Abstracted in Dissertation abstracts, v. 19 (1959) no. 11, p. 2745-2746. Vita. eContent provider-neutral record in process. Description based on print version record. Includes bibliographical references.
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Neuroelectrical Investigations Into the Sensory and Cognitive Effects of Nicotine and Monoamine Oxidase Inhibition in HumansSmith, Dylan January 2015 (has links)
Investigations into the cognitive effects of tobacco smoking have generally focused on nicotine and its effect on nicotinic acetylcholine receptors (nAChRs) in the brain. However, it is now known that chronic smokers exhibit robust inhibition of the monoamine oxidase (MAO) enzyme through the actions of non-nicotine components in tobacco smoke. Therefore, the primary aim of this thesis is to elucidate the effects of nicotine and MAO-inhibition on electroencephalographic (EEG) and event-related potential (ERP) measures of cognition. 24 healthy nonsmoking males were administered 75 mg of moclobemide, and chewed 6 mg nicotine gum, in order to simulate the effects of acute smoking. Four experimental conditions included placebo, nicotine, moclobemide, and a combination of nicotine and moclobemide. Early auditory ERPs were used as measures of cognition, such as the auditory P50 sensory gating paired-stimulus paradigm, the acoustic-change-elicited mismatch-negativity (MMN), the novel sound-elicited P3a, and the target sound-elicited P3b. Three minutes of eyes closed EEG were also recorded. Because these ERPs are often identified as biomarkers for schizophrenia, drug effects were also measured after individuals were stratified for low-baseline amplitude of each ERP measure, as a laboratory model of cognitive deficits in schizophrenia. Overall results showed a synergistic improvement in sensory gating via nicotine combined with moclobemide, accompanied by a reduction in theta band power. Nicotine in the absence of moclobemide increased P3b amplitude, accompanied by an increase in alpha2 band power. Moclobemide in the absence of nicotine increased P3a amplitude, accompanied by a decrease in beta2 power. Stratifying participants by placebo amplitude revealed both nicotine and moclobemide exhibited an inverted-U pattern of effect, i.e. showing greater amplitude increases in individuals with the lowest baseline amplitudes. Overall, this thesis demonstrates how these two components of tobacco smoke affect different facets of auditory processing in different ways, with synergistic effects in some paradigms but antagonizing effects in others. Therefore, chronic smokers and schizophrenia patients who seek transient cognitive improvement through smoking may actually experience cognitive detriments overall, possibly contributing to withdrawal symptoms and/or an exacerbation of already-present psychiatric symptoms.
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