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Dive into the research topics where J Meyer is active.

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Featured researches published by J Meyer.


European Journal of Nuclear Medicine and Molecular Imaging | 2000

Imaging the serotonin transporter with positron emission tomography: initial human studies with [11C]DAPP and [11C]DASB

Sylvain Houle; Nathalie Ginovart; Douglas Hussey; J Meyer; Alan A. Wilson

Abstract. Two novel radioligands, N,N-dimethyl-2-(2-amino-4-methoxyphenylthio)benzylamine (DAPP) and (N,N-dimethyl-2-(2-amino-4-cyanophenylthio)benzylamine (DASB), were radiolabeled with carbon-11 and evaluated as in vivo probes of the serotonin transporter (SERT) using positron emission tomography (PET). Both compounds are highly selective, with nanomolar affinity for the serotonin transporter and micromolar affinity for the dopamine and norepinephrine transporters. Six volunteers were imaged twice, once with each of the two radioligands. Both ligands displayed very good brain penetration and selective retention in regions rich in serotonin reuptake sites. Both had similar brain uptake and kinetics, but the cyano analogue, [11C]DASB, had a slightly higher brain penetration in all subjects. Plasma analysis revealed that both radiotracers were rapidly metabolized to give mainly hydrophilic species as determined by reverse-phase high-performance liquid chromatography. Inhibition of specific binding to the SERT was demonstrated in three additional subjects imaged with [11C]DASB following an oral dose of the selective serotonin reuptake blocker citalopram. These preliminary studies indicate that both these substituted phenylthiobenzylamines have highly suitable characteristics for probing the serotonin reuptake system with PET in humans.


Journal of Medicinal Chemistry | 2000

Novel Radiotracers for Imaging the Serotonin Transporter by Positron Emission Tomography: Synthesis, Radiosynthesis, and in Vitro and ex Vivo Evaluation of (11)C-Labeled 2-(Phenylthio)araalkylamines.

Alan A. Wilson; Nathalie Ginovart; Mark Schmidt; J Meyer; Sylvain Houle

A series of four 2-(phenylthio)araalkylamines have been radiolabeled with 11C and evaluated as potential radiotracers for imaging the serotonin transporter (SERT) by positron emission tomography (PET). All four candidates display high affinity for SERT and low affinity for the dopamine or norepinephrine transporters using in vitro binding assays. Biodistribution studies in rats demonstrated that tail-vein injection of the 11C-labeled radiotracers resulted in high brain uptake of radioactivity with a preferential distribution in brain regions known to be rich in SERT such as hypothalamus and thalamus. The most promising candidate, 16, had hypothalamus-to-cerebellum ratios of 9:1, 1 h postinjection, an indication of high specific to nonspecific binding. Ex vivo pharmacological studies demonstrated that uptake in SERT-rich brain regions was both saturable and selective for SERT. Two of the tested radiotracers, 15 and 16, have highly favorable properties for imaging SERT and will be used in pilot human PET im...


Nuclear Medicine and Biology | 2003

Synthesis and in vivo evaluation of novel radiotracers for the in vivo imaging of the norepinephrine transporter.

Alan A. Wilson; David Patrick Johnson; David Mozley; Doug Hussey; Nathalie Ginovart; José N. Nobrega; Armando Garcia; J Meyer; Sylvain Houle

The (R,R) and (S,S) enantiomers of 2-[(2-methoxyphenoxy)phenylmethyl]morpholine (MeNER) have been radiolabelled with carbon-11 in good yield and at high specific activity. These radiotracers are close analogues of reboxetine, a potent and selective ligand for the norepinephrine transporter (NET). They were examined as potential ligands for imaging NET in vivo by positron emission tomography (PET). The in vivo brain distribution of both [(11)C]-labeled enantiomers were evaluated in rats. Following tail-vein injection of the (R,R)-enantiomer regional brain uptake and washout of radioactivity was homogeneous at all time points examined (5-60 min). In contrast, administration of the (S,S)-enantiomer produced a heterogeneous distribution of radioactivity in brain with highest uptake in the hypothalamus, a NET rich region, and lowest uptake in the striatum, a brain region devoid of NET. Hypothalamus to striatum ratios of 2.5 to one were achieved at 60 min post injection of (S,S)-[(11)C]-MeNER. Pre-injection of the norepinephrine reuptake inhibitors, reboxetine or desipramine, reduced hypothalamus to striatum ratios to near unity while reuptake inhibitors of dopamine and serotonin had no significant effect on binding. In vitro autoradiography studies (rat brain slices) with (S,S)-[(11)C]-MeNER produced a regional distribution pattern that was consistent with the reported distribution of NET. (S,S)-[(11)C]-MeNER has the potential to be the first successful PET ligand to image NET.


Psychological Medicine | 2011

Relationship of monoamine oxidase A binding to adaptive and maladaptive personality traits

Alexandra Soliman; R. M. Bagby; Alan A. Wilson; Laura Miler; Michael Clark; Pablo Rusjan; Julia Sacher; Sylvain Houle; J Meyer

BACKGROUND Monoamine oxidase A (MAOA) is an important enzyme that metabolizes monoamines such as serotonin, norepinephrine and dopamine in the brain. In prefrontal cortex, low MAOA binding is associated with aggression and high binding is associated with major depressive disorder (MDD) and also risk for recurrence of depressive episodes. In rodent models, low MAOA levels are associated with increased aggression and fear conditioning, and decreased social and exploratory investigative behaviors. Our objective was to measure MAOA binding in prefrontal cortex and concurrently evaluate a broad range of validated personality traits. We hypothesized that prefrontal MAOA binding would correlate negatively with angry-hostility, a trait related to aggression/anger, and positively with traits intuitively related to adaptive investigative behavior. METHOD Participants were aged 19-49 years, healthy and non-smoking. MAOA binding was measured with [11C]harmine positron emission tomography (PET) in prefrontal brain regions and personality traits were measured with the NEO Personality Inventory Revised (NEO PI-R). RESULTS Prefrontal MAOA binding correlated negatively with angry-hostility (r=-0.515, p=0.001) and positively with deliberation (r=0.514, p=0.001). In a two-factor regression model, these facets explained 38% of variance in prefrontal MAOA binding. A similar relationship was found in prefrontal cortex subregions. CONCLUSIONS We propose a new continuum describing the relationship between personality and MAOA: deliberate/thoughtful contrasting aggressive/impulsive. Additionally, the association between high MAOA binding and greater deliberation may explain why some people have moderately high levels of MAOA, although very high levels occur during MDD. In health, higher MAOA binding is associated with an adaptive personality facet.


Acta Psychiatrica Scandinavica | 2015

Light therapy and serotonin transporter binding in the anterior cingulate and prefrontal cortex

S. J. Harrison; A. E. Tyrer; Robert D. Levitan; Xin Xu; Sylvain Houle; Alan A. Wilson; José N. Nobrega; Pablo Rusjan; J Meyer

To investigate the effects of light therapy on serotonin transporter binding (5‐HTT BPND), an index of 5‐HTT levels, in the anterior cingulate and prefrontal cortices (ACC and PFC) of healthy individuals during the fall and winter. Twenty‐five per cent of healthy individuals experience seasonal mood changes that affect functioning. 5‐HTT BPND has been found to be higher across multiple brain regions in the fall and winter relative to spring and summer, and elevated 5‐HTT BPND may lead to extracellular serotonin loss and low mood. We hypothesized that, during the fall and winter, light therapy would reduce 5‐HTT BPND in the ACC and PFC, which sample brain regions involved in mood regulation.


NeuroImage | 2008

Recent advances towards imaging cerebral β-adrenergic receptors with PET

Neil Vasdev; Karin A. Stephenson; E.M. van Oosten; J Meyer; Sylvain Houle; Alan A. Wilson

Introduction: Imaging cerebral β-Adrenergic receptors (βARs) with PET remains elusive in humans due to the lack of a suitable radiotracer. Our goal was to develop general synthetic and radiosynthetic methods amenable to the preparation of small libraries of novel Fand F-labelled β-blockers. We report our preliminary cerebral ex vivo biodistribution studies of new [F]-labelled β-blockers, prepared via efficient synthetic methodologies, in rodents.


NeuroImage | 2008

Serotonin transporter occupancy by citalopram treatment in geriatric depression

G. Smith; Alan Kahn; K Hanratty; Julia Sacher; J Meyer; Pablo Rusjan; Alan A. Wilson; Alastair J. Flint; Benoit H. Mulsant; Sylvain Houle


Archive | 2009

Neurochemical aspects of porstpartum mood changes: a time course of monoamine oxidase a levels during the postpartum period

Julia Sacher; Alan A. Wilson; Sylvain Houle; Sabrina Hassan; Donna E. Stewart; Pablo Rusjan; J Meyer


Archive | 2009

Prefrontal cortex MAO-A binding in cigarette smokers under acute abstinence

Ingrid Bacher; Sylvain Houle; Tony P. George; Peter Selby; Alan A. Wilson; Julia Sacher; Bin Wu; J Meyer


Archive | 2008

Serotonin transporter occupancy of high dose serotonin reuptake inhibitor antidepressants in major depressive disorder

Aristotle N. Voineskos; Julia Sacher; Alan A. Wilson; Sylvain Houle; Robert D. Levitan; K Chopra; Pablo Rusjan; J Meyer

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Alan A. Wilson

Centre for Addiction and Mental Health

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Sylvain Houle

Centre for Addiction and Mental Health

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Pablo Rusjan

Centre for Addiction and Mental Health

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Julia Sacher

Centre for Addiction and Mental Health

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José N. Nobrega

Centre for Addiction and Mental Health

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Nathalie Ginovart

Centre for Addiction and Mental Health

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Robert D. Levitan

Centre for Addiction and Mental Health

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Sabrina Hassan

Centre for Addiction and Mental Health

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Julia Sacher

Centre for Addiction and Mental Health

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