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海马体体积未减小与患精神病的较高风险相关。

Non-reduction in hippocampal volume is associated with higher risk of psychosis.

作者信息

Phillips Lisa J, Velakoulis Dennis, Pantelis Christos, Wood Stephen, Yuen Hok Pan, Yung Alison R, Desmond Patricia, Brewer Warrick, McGorry Patrick D

机构信息

PACE Clinic, Department of Psychiatry, University of Melbourne, 35 Poplar Road, Victoria 3052, Parkville, Australia.

出版信息

Schizophr Res. 2002 Dec 1;58(2-3):145-58. doi: 10.1016/s0920-9964(01)00392-9.

Abstract

Previous research using MRI scans has shown reduced hippocampal volumes in chronic schizophrenia and first-episode psychosis compared to well subjects. There are few MRI volumetric studies of high-risk cohorts and no studies that have compared structural measures between high-risk subjects who later developed a psychotic illness and those who did not. Therefore, the question of whether structural changes to the hippocampi precede the onset of an acute psychotic episode has not been answered. Hippocampal and whole brain volumes of 60 people at ultra high-risk (UHR) of developing a psychotic episode (identified through state and trait criteria) were obtained through MRI scan and compared with subjects with first episode psychosis (FEP: n=32), and no mental illness (n=139). Thirty-three percent (n=20) of the UHR cohort developed a psychotic disorder during the 12-month period following the MRI scan. The UHR group as a whole, like the FEP group, had significantly smaller left and right hippocampal volumes than the normal comparison group. Contrary to our initial hypothesis, the left hippocampal volume of the UHR subjects who developed a psychotic disorder was larger than the UHR-non-psychotic subgroup and the FEP group, but no differences were found between the UHR-psychotic and normal groups. The right hippocampus of the UHR-non-psychotic group was significantly smaller than the Normal group but not different to the FEP group. Furthermore, a larger left hippocampal volume of the UHR cohort at intake was associated with the subsequent development of acute psychosis rather than smaller volumes. These results contradicted the expected outcomes, which had been influenced by the neurodevelopmental model of the development of psychosis and an earlier study comparing hippocampal volumes of first episode, chronic schizophrenia and normal populations. One implication of these results is that a process of dynamic central nervous system change may occur during the onset phase of schizophrenia and related disorders, rather than earlier in life as suggested by the neurodevelopmental model. Alternatively, selection factors associated with the UHR cohort may have created a bias in the results. Replication of these results is required in other high-risk cohorts.

摘要

以往使用磁共振成像(MRI)扫描的研究表明,与健康受试者相比,慢性精神分裂症患者和首发精神病患者的海马体体积减小。针对高危人群的MRI体积研究较少,且尚无研究比较后来发展为精神病性疾病的高危受试者与未发展为精神病性疾病的高危受试者之间的结构测量结果。因此,海马体的结构变化是否先于急性精神病发作这一问题尚未得到解答。通过MRI扫描获取了60名处于发展为精神病性发作超高风险(UHR)状态(通过状态和特质标准确定)的人的海马体和全脑体积,并与首发精神病患者(FEP:n = 32)和无精神疾病的受试者(n = 139)进行比较。在MRI扫描后的12个月内,33%(n = 20)的UHR队列发展为精神病性障碍。与FEP组一样,UHR组整体的左右海马体体积明显小于正常对照组。与我们最初的假设相反,发展为精神病性障碍的UHR受试者的左侧海马体体积大于UHR非精神病亚组和FEP组,但UHR精神病组与正常组之间未发现差异。UHR非精神病组的右侧海马体明显小于正常组,但与FEP组无差异。此外,UHR队列在纳入时左侧海马体体积较大与随后急性精神病的发展相关,而非较小体积。这些结果与预期结果相矛盾,预期结果受到精神病发展的神经发育模型以及一项比较首发、慢性精神分裂症和正常人群海马体体积的早期研究的影响。这些结果的一个含义是,在精神分裂症及相关疾病的发作阶段可能会发生动态中枢神经系统变化过程,而不是如神经发育模型所暗示的在生命早期发生。或者,与UHR队列相关的选择因素可能在结果中造成了偏差。其他高危队列需要重复这些结果。

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