4.7 Article

Early striatal hypertrophy in first-episode psychosis within 3 weeks of initiating antipsychotic drug treatment

Journal

PSYCHOLOGICAL MEDICINE
Volume 39, Issue 5, Pages 793-800

Publisher

CAMBRIDGE UNIV PRESS
DOI: 10.1017/S0033291708004212

Keywords

Antipsychotic; brain; first episode; MRI; schizophrenia

Funding

  1. University of Hong Kong Committee for Conference and Research Grants (CRCG)

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Background. We and others have reported that patients experiencing their first episode of psychosis already have significant structural brain abnormalities. Antipsychotics seem to reverse subcortical volume deficits after months of treatment. However, the early, impact of medication on brain morphology is not known. Method. Forty-eight individuals in their first episode of psychosis underwent magnetic resonance imaging (MRI) brain scanning. Twenty-six were antipsychotic naive and 22 were newly treated with antipsychotic medication for I two groups a median period of 3 weeks. In each group, 80%, of subjects received a diagnosis of schizophrenia. The were balanced for age, sex, handedness, ethnicity, height, years of education, paternal socio-economic Status (SES) and Positive and Negative Syndrome Scale (PANSS) score. Group differences in whole-brain grey matter were compared voxel by voxel, using Brain Activation and Morphological Mapping (BAMM) software. We also conducted testing of group differences with region-of-interest (ROI) measurements of the caudate nucleus. Results. Relative to the untreated group, those receiving antipsychotic medication for 3-4 weeks had significantly greater grey-matter Volumes in the bilateral caudate and cingulate gyri, extending to the left medial frontal gyros. ROI analysis confirmed that, in treated patients, the right and left caudate nuclei were significantly larger by 10%, (p<0.039, two-tailed) and 9%, (p<0.048, two-tailed) respectively. Conclusions. Early striatal grey-matter enlargement may occur within the first 3-4, weeks of antipsychotic treatment. Possible reasons for putative striatal hypertrophy and its implications are discussed.

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