Circuit-based framework for understanding neurotransmitter and risk gene interactions in schizophrenia

Lisman, John; Coyle, Joseph T.; Green, Robert W.; Javitt, Daniel C.; Beneš, Francine M.; Heckers, Stephan; Grace, Anthony A.

doi:10.1016/j.tins.2008.02.005

Cited by 894 publications

(859 citation statements)

References 161 publications

(161 reference statements)

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“…This leads to a longer time constant of the calcium decay after a spike in the interneuron. It has been proposed that the reduction of PV in Schizophrenia is a compensatory mechanism which aims to increase the gain of the interneurons and therefore the inhibition (Lisman et al, 2008). However, we have shown in the GENE-SIS model that the longer inhibition by the Ca dynamics has no influence on the STDP curve.…”

Section: Discussionmentioning

confidence: 57%

“…This means that on the network level less NMDA activation will lead to more activity. This has been recently pointed out by Lisman et al (2008) who proposes that cells in fact reduce their PV concentration to "fake" the longer NMDA activation in interneurons. While this has no effect on the STDP curve this is an important property for network stability which leads to the last point, namely network effects.…”

Section: Discussionmentioning

confidence: 89%

“…Virtually all modern hypotheses about Schizophrenia focus on the hypofunction of inhibitory neurons in the prefrontal cortex (Paz et al, 2008;Lisman et al, 2008;Lewis et al, 2005). However there are conflicting views on which defect in the inhibitory neurons is responsible for its hypofunction.…”

Section: Discussionmentioning

confidence: 99%

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How feedback inhibition shapes spike-timing-dependent plasticity and its implications for recent Schizophrenia models

et al. 2011

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It has been shown that plasticity is not a fixed property but, in fact, changes depending on the location of the synapse on the neuron and/or changes of biophysical parameters. Here we investigate how plasticity is shaped by feedback inhibition in a cortical microcircuit. We use a differential Hebbian learning rule to model spike-timing dependent plasticity and show analytically that the feedback inhibition shortens the time window for LTD during spike-timing dependent plasticity but not for LTP. We then use a realistic GENESIS model to test two hypothesis about interneuron hypofunction and conclude that a reduction in GAD67 is the most likely candidate as the cause for hypofrontality as observed in Schizophrenia.

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Section: Discussionmentioning

confidence: 57%

Section: Discussionmentioning

confidence: 89%

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How feedback inhibition shapes spike-timing-dependent plasticity and its implications for recent Schizophrenia models

et al. 2011

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“…This regimen also elicits alterations in N-acetylaspartate (NAA) and N-acetylaspartylglutamate (NAAG) in temporal cortex and hippocampus (Reynolds et al, 2005), and decreases 5HT2A receptor binding in the PFC (Steward et al, 2004) in close similarity to schizophrenia pathology (Laruelle et al, 1993;Nudmamud et al, 2003). Furthermore, while the behavioral and neurochemical effects of acute exposures to NMDA-R antagonists are believed to occur upon disinhibition of cortical excitatory activity due to increased sensitivity of inhibitory systems to blockade of NMDA-R function (Olney et al, 1999;Homayoun and Moghaddam, 2007;Lisman et al, 2008;Middleton et al, 2008), they do not lead to the enduring changes in PV-interneurons observed in schizophrenia. Repetitive exposures to NMDA-R antagonists, on the other hand, produce a reduction in GAD67 expression in PVinterneurons of rodents (Behrens et al, 2007 as well as decreased expression of parvalbumin in rodents and non-human primates (Cochran et al, 2002;Keilhoff et al, 2004;Rujescu et al, 2006;Morrow et al, 2007).…”

Section: Introductionmentioning

confidence: 99%

Does schizophrenia arise from oxidative dysregulation of parvalbumin-interneurons in the developing cortex?

2009

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An imbalance in the redox-state of the brain may be part of the underlying pathophysiology in schizophrenia. Inflammatory mediators, such as IL-6, which can tip the redox balance into a prooxidant state, have been consistently found to be altered in schizophrenia patients. However, the relationship of altered redox-state to altered brain functions observed in the disease has been unclear. Recent data from a pharmacological model of schizophrenia suggest that redox and inflammatory imbalances may be directly linked to the pathophysiology of the disease by alterations in fast-spiking interneurons. Repetitive adult-exposure to the NMDA-R antagonist ketamine increases the levels of the proinflammatory cytokine interleukin-6 in brain which, through activation of the superoxide-producing enzyme NADPH-oxidase (Nox2), leads to the loss of the GABAergic phenotype of PV-interneurons and to decreased inhibitory activity in prefrontal cortex. This effect is not observed after a single exposure to ketamine, suggesting that the first exposure to the NMDA-R antagonist primes the brain such that deleterious effects on PVinterneurons appear upon repetitive exposures. The effects of activation of the IL-6/Nox2 pathway on the PV-interneuronal system are reversible in the adult brain, but permanent in the developing cortex. The slow development of PV-interneurons, while essential for shaping of neuronal circuits during postnatal brain development, increases their vulnerability to deleterious insults that can permanently affect their maturational process. Thus, in individuals with genetic predisposition, the persistent activation of the IL-6/Nox2 pathway may be an environmental factor that tips the redoxbalance leading to schizophrenia symptoms in late adolescence and early adulthood.

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“…Alternativement, un composé qui se lierait au NTD des sous-unités GluN2 et en empêcherait la fermeture devrait aussi permettre une potentialisation des récepteurs NMDA [34]. De tels modulateurs positifs pourraient être utiles dans le cadre de thé-rapies contre des psychoses telles que la schizophrénie étant donné l'implication probable d'un déficit d'activité des récepteurs NMDA dans ces pathologies [39]. Au contraire, des inhibiteurs des récepteurs NMDA pourraient aider à lutter contre des pathologies impliquant une suractivité de ces récepteurs, par exemple lors d'ischémies cérébrales consécutives à un accident vasculaire cérébral [28], ou encore dans le cas de douleurs neuropathiques [7].…”

Section: Perspectives Pharmacologiquesunclassified

Fonctionnement des récepteurs-canaux du glutamate

Gielen¹

2010

Med Sci (Paris)

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Dans le cerveau des vertébrés, le glutamate est le principal neurotransmetteur excitateur. Ainsi, à la majorité des synapses excitatrices, le glutamate diffuse dans la fente synaptique après sa libération vésiculaire par le neurone présynaptique (Figure 1). Deux grandes classes de récepteurs sont alors activées : les récepteurs métabotropiques du glutamate (mGluR), couplés à des protéines G, et les récepteurs-canaux du glutamate (ou encore récepteurs ionotropiques du glutamate, iGluR), contenant un canal ionique perméable aux cations (Na + et K + , mais aussi, dans certains cas, Ca 2+ , un messager intracellulaire majeur ; voir ci-dessous) (Figure 1). L'activation des iGluR est donc à l'origine d'un flux ionique à travers la membrane plasmique du neurone postsynaptique qui provoque sa dépolarisation et peut ainsi permettre l'initiation de potentiels d'action. Les mGluR ne peuvent répondre qu'à des expositions prolongées au glutamate, par exemple lors de libérations répétées de glutamate dues à des trains de potentiels > Les récepteurs-canaux du glutamate (iGluR) sont responsables de la transmission synaptique excitatrice rapide dans le cerveau des verté-brés. Les différentes familles d'iGluR (récepteurs AMPA, kaïnate et NMDA) ont une organisation moléculaire semblable, divers domaines d'origine bactérienne ayant été assemblés au cours de l'évolution pour façonner une architecture commune. Durant la dernière décennie, les apports complémentaires de la cristallographie et de l'électrophysiologie ont permis des avancées majeures dans la compréhension des mécanis-mes moléculaires qui régissent l'activation et la modulation des iGluR. Cette revue présente ces mécanismes et montre en quoi une connaissance détaillée du fonctionnement des iGluR permet d'appréhender leur rôle au niveau de la synapse excitatrice, mais également leur potentiel comme cibles d'intérêt thérapeutique dans le traitement de certaines pathologies neurologiques ou psychiatriques. <

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Circuit-based framework for understanding neurotransmitter and risk gene interactions in schizophrenia

Cited by 894 publications

References 161 publications

How feedback inhibition shapes spike-timing-dependent plasticity and its implications for recent Schizophrenia models

How feedback inhibition shapes spike-timing-dependent plasticity and its implications for recent Schizophrenia models

Does schizophrenia arise from oxidative dysregulation of parvalbumin-interneurons in the developing cortex?

Fonctionnement des récepteurs-canaux du glutamate

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