Mechanism of action of antipsychotic drugs : From dopamine D2 receptor antagonism to glutamate NMDA facilitation

Abstract The fundamental pathologic processes associated with schizophrenia remain uncertain. The goal of this article was to review imaging evidence suggesting that schizophrenia is associated with excessive stimulation of D2 receptors, as well as imaging experiments supporting the hypothesis that...

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Published inClinical therapeutics Vol. 27; pp. S16 - S24
Main Authors LARUELLE, Marc, FRANKLE, W. Gordon, NARENDRAN, Rajesh, KEGELES, Lawrence S, ABI-DARGHAM, Anissa
Format Conference Proceeding Journal Article
LanguageEnglish
Published Belle Mead, NJ Excerpta Medica 2005
Elsevier Limited
Subjects
Amphetamines
Antipsychotics
Biological and medical sciences
Dopamine
Drug dosages
Ketamine
Medical sciences
Pathogenesis
Pathophysiology
Pharmacology. Drug treatments
Psychiatry
Psychopharmacology
Psychosis
Psychotropic drugs
Schizophrenia
Tomography
Trends
Radionuclide study
Facilitation
Drug
Dopamine
Neuroleptic
Schizophrenia
Catecholamine
Glutamate
Psychosis
Antagonism
D2 Dopamine receptor
Excitatory aminoacid
Neurotransmitter
NMDA
Antipsychotic
Mechanism of action
Positron emission tomography
PET
single-photon emission computed tomography
Positron
Emission tomography
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Summary:Abstract The fundamental pathologic processes associated with schizophrenia remain uncertain. The goal of this article was to review imaging evidence suggesting that schizophrenia is associated with excessive stimulation of D2 receptors, as well as imaging experiments supporting the hypothesis that this dysregulation might be secondary to N - methyl-d-aspartate (NMDA) dysfunction. Recent imaging data support the association of schizophrenia with a dopamine endophenotype involving excessive subcortical dopamine function. Animal and imaging data are consistent with the idea that this abnormality might be secondary to a synaptic disconnectivity involving the prefrontal cortex, which is well modeled by NMDA antagonist administration. In turn, this dopamine dysregulation might worsen synaptic connectivity and NMDA function. Thus, both glutamate/dopamine and dopamine/glutamate interactions may be relevant to schizophrenia pathophysiology and treatment. A deficit in glutamate transmission may lead to the dopamine endophenotype associated with this illness, and dopamine alterations in turn might exacerbate glutamate transmission deficits. The view that NMDA alterations are primary and dopamine alterations are secondary is probably oversimplistic, as both sets of abnormalities reinforce each other. A consequence of this general model is that direct intervention to support NMDA function might be beneficial as an augmentation strategy for the treatment of schizophrenia. Thus, it is proposed that schizophrenia is associated with strongly interconnected abnormalities of glutamate and dopamine transmission: NMDA hypofunction in the prefrontal cortex and its connections might generate a pattern of dysregulation of dopamine systems that, in turn, further weakens NMDA-mediated connectivity and plasticity.
ISSN:0149-2918
1879-114X
DOI:10.1016/j.clinthera.2005.07.017