The contribution of first-episode illness characteristics and cumulative antipsychotic usage to progressive structural brain changes over a long-term follow-up in schizophrenia

IF 2.1 4区 医学 Q3 CLINICAL NEUROLOGY Psychiatry Research: Neuroimaging Pub Date : 2024-01-29 DOI:10.1016/j.pscychresns.2024.111790
Tuomas Konttajärvi , Marianne Haapea , Sanna Huhtaniska , Lassi Björnholm , Jouko Miettunen , Matti Isohanni , Matti Penttilä , Graham K. Murray , Hannu Koponen , Anthony C. Vernon , Erika Jääskeläinen , Johannes Lieslehto
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Abstract

Exposure to antipsychotics as well as certain first-episode illness characteristics have been associated with greater gray matter (GM) deficits in the early phase of schizophrenia. Whether the first-episode illness characteristics affect the long-term progression of the structural brain changes remain unexplored. We therefore assessed the role of first-episode illness characteristics and life-time antipsychotic use in relation to long-term structural brain GM changes in schizophrenia. Individuals with schizophrenia (SZ, n = 29) and non-psychotic controls (n = 61) from the Northern Finland Birth Cohort 1966 underwent structural MRI at the ages of 34 (baseline) and 43 (follow-up) years. At follow-up, the average duration of illness was 19.8 years. Voxel-based morphometry was used to assess the effects of predictors on longitudinal GM changes in schizophrenia-relevant brain areas. Younger age of onset (AoO), higher cumulative antipsychotic dose and severity of symptoms were associated with greater GM deficits in the SZ group at follow-up. None of the first-episode illness characteristics were associated with longitudinal GM changes during 9-year follow-up period. We conclude that a younger AoO and high life-time antipsychotic use may contribute to progression of structural brain changes in schizophrenia. Apart from AoO, other first-episode illness characteristics may not contribute to longitudinal GM changes in midlife.

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精神分裂症患者首次发病特征和累计使用抗精神病药物对长期随访期间大脑结构渐进性变化的影响
在精神分裂症的早期阶段,抗精神病药物的接触以及某些首发疾病的特征与灰质(GM)缺陷的加重有关。首次发病的疾病特征是否会影响大脑结构变化的长期进展仍有待研究。因此,我们评估了首发疾病特征和终生服用抗精神病药物对精神分裂症患者大脑结构基因组长期变化的影响。来自1966年北芬兰出生队列的精神分裂症患者(SZ,n = 29)和非精神分裂症对照组(n = 61)分别在34岁(基线)和43岁(随访)时接受了结构磁共振成像检查。随访时的平均病程为 19.8 年。研究人员使用体素形态计量法评估了预测因素对精神分裂症相关脑区纵向基因组变化的影响。发病年龄(AoO)较小、抗精神病药物累积剂量较高和症状严重程度较高与随访时精神分裂症组的基因组缺损较严重有关。在9年的随访期间,首次发病的疾病特征均与GM的纵向变化无关。我们的结论是,较年轻的AoO和终生大量使用抗精神病药物可能会导致精神分裂症患者大脑结构变化的进展。除了急性发作期,其他首次发病的疾病特征可能不会导致中年期大脑结构的纵向变化。
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来源期刊
Psychiatry Research: Neuroimaging
Psychiatry Research: Neuroimaging 医学-精神病学
CiteScore
3.80
自引率
0.00%
发文量
86
审稿时长
22.5 weeks
期刊介绍: The Neuroimaging section of Psychiatry Research publishes manuscripts on positron emission tomography, magnetic resonance imaging, computerized electroencephalographic topography, regional cerebral blood flow, computed tomography, magnetoencephalography, autoradiography, post-mortem regional analyses, and other imaging techniques. Reports concerning results in psychiatric disorders, dementias, and the effects of behaviorial tasks and pharmacological treatments are featured. We also invite manuscripts on the methods of obtaining images and computer processing of the images themselves. Selected case reports are also published.
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