Progression from selective to general involvement of hippocampal subfields in schizophrenia

被引:0
|
作者
N F Ho
J E Iglesias
M Y Sum
C N Kuswanto
Y Y Sitoh
J De Souza
Z Hong
B Fischl
J L Roffman
J Zhou
K Sim
D J Holt
机构
[1] Institute of Mental Health,Research Division
[2] Center for Cognitive Neuroscience,Department of Neuroradiology
[3] Neuroscience and Behavioral Disorders Program,Department of Radiology
[4] Duke-National University of Singapore Graduate Medical School,Department of Psychiatry
[5] Basque Center on Cognition,Department of General Psychiatry
[6] Brain and Language,undefined
[7] AA Martinos Center for Biomedical Imaging,undefined
[8] Massachusetts General Hospital,undefined
[9] National Neuroscience Institute,undefined
[10] Harvard Medical School,undefined
[11] Massachusetts General Hospital,undefined
[12] Harvard Medical School,undefined
[13] General Psychiatry,undefined
[14] Institute of Mental Health,undefined
来源
Molecular Psychiatry | 2017年 / 22卷
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摘要
Volume deficits of the hippocampus in schizophrenia have been consistently reported. However, the hippocampus is anatomically heterogeneous; it remains unclear whether certain portions of the hippocampus are affected more than others in schizophrenia. In this study, we aimed to determine whether volume deficits in schizophrenia are confined to specific subfields of the hippocampus and to measure the subfield volume trajectories over the course of the illness. Magnetic resonance imaging scans were obtained from Data set 1: 155 patients with schizophrenia (mean duration of illness of 7 years) and 79 healthy controls, and Data set 2: an independent cohort of 46 schizophrenia patients (mean duration of illness of 18 years) and 46 healthy controls. In addition, follow-up scans were collected for a subset of Data set 1. A novel, automated method based on an atlas constructed from ultra-high resolution, post-mortem hippocampal tissue was used to label seven hippocampal subfields. Significant cross-sectional volume deficits in the CA1, but not of the other subfields, were found in the schizophrenia patients of Data set 1. However, diffuse cross-sectional volume deficits across all subfields were found in the more chronic and ill schizophrenia patients of Data set 2. Consistent with this pattern, the longitudinal analysis of Data set 1 revealed progressive illness-related volume loss (~2–6% per year) that extended beyond CA1 to all of the other subfields. This decline in volume correlated with symptomatic worsening. Overall, these findings provide converging evidence for early atrophy of CA1 in schizophrenia, with extension to other hippocampal subfields and accompanying clinical sequelae over time.
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页码:142 / 152
页数:10
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