Glutamate levels and symptom burden in high-risk and first-episode schizophrenia: a dual-voxel study of the anterior cingulate cortex.

IF 4.1 2区 医学 Q2 NEUROSCIENCES Journal of Psychiatry & Neuroscience Pub Date : 2024-11-14 Print Date: 2024-11-01 DOI:10.1503/jpn.240094
Lejia Fan, Zhenmei Zhang, Xiaoqian Ma, Liangbing Liang, Yujue Wang, Liu Yuan, Lijun Ouyang, Zongchang Li, Xiaogang Chen, Ying He, Lena Palaniyappan
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Abstract

Background: Reduced glutamatergic excitability of the anterior cingulate cortex (ACC) has been long suspected in schizophrenia; recent observations support low glutamatergic tone as the primary pathophysiology contributing to subtle early features of this illness, with a secondary disinhibition (higher glutamate tone) resulting in more prominent clinical symptoms later in its course. We sought to investigate whether people with genetic high risk (GHR) for schizophrenia have lower glutamate levels in the ACC than those at later stages of clinical high risk (CHR) and those with first-episode schizophrenia (FES), among whom symptoms are already prominent.

Methods: We recruited people with CHR, GHR, or FES, as well as healthy controls. Using proton magnetic resonance spectroscopy, we determined glutamate levels in the perigenual ACC (pACC) and dorsal ACC (dACC) using a 3 T scanner.

Results: We recruited 302 people across multiple stages of psychosis, including 63 with CHR, 76 with GHR, and 96 with FES, as well as 67 healthy controls. Those with GHR had lower glutamate levels in the dACC than those with CHR, while those with CHR had higher glutamate levels in the pACC than those with FES. Higher disorganization, but not any other symptom domain, was associated with lower levels of glutamate in the GHR group (dACC and pACC) and in the CHR group (pACC).

Limitations: The cross-sectional design precluded inferences regarding individual clinical trajectory and resolution at 3 T was insufficient to separate spectra of glutamine from glutamate.

Conclusion: Reduced glutamatergic tone among people genetically predisposed to schizophrenia supports diminished excitability as an early feature of schizophrenia, contributing to the subtle symptom of disorganization across high-risk states. Higher glutamate levels become apparent when psychotic symptoms become prominent, possibly as a disinhibitory effect and, at the full-blown stage of psychosis, the relationship between glutamate concentrations and symptoms ceases to be simply linear.

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高危和首发精神分裂症患者的谷氨酸水平和症状负担:前扣带回皮层双象素研究。
背景:长期以来,人们一直怀疑前扣带回皮层(ACC)的谷氨酸能兴奋性降低与精神分裂症有关;最近的观察结果表明,谷氨酸能张力低是导致该病早期微妙特征的主要病理生理学因素,而继发性抑制(谷氨酸张力较高)则会在病程后期导致更突出的临床症状。我们试图研究精神分裂症遗传高危人群(GHR)的ACC谷氨酸水平是否低于临床高危后期人群(CHR)和首发精神分裂症患者(FES),因为后者的症状已经很突出:我们招募了CHR、GHR或FES患者以及健康对照者。通过质子磁共振波谱,我们使用 3 T 扫描仪测定了本源 ACC 周围(pACC)和背侧 ACC(dACC)的谷氨酸水平:我们招募了 302 名不同阶段的精神病患者,包括 63 名 CHR 患者、76 名 GHR 患者和 96 名 FES 患者,以及 67 名健康对照者。GHR患者的dACC谷氨酸水平低于CHR患者,而CHR患者的pACC谷氨酸水平高于FES患者。在GHR组(dACC和pACC)和CHR组(pACC)中,较高的无组织性与较低的谷氨酸水平相关,但与其他症状领域无关:局限性:横断面设计排除了对个体临床轨迹的推断,3 T 的分辨率不足以分离谷氨酰胺和谷氨酸的光谱:在精神分裂症遗传易感人群中,谷氨酸能张力的降低支持了兴奋性降低是精神分裂症的早期特征,有助于在高危状态下出现细微的紊乱症状。当精神病症状变得突出时,谷氨酸水平会明显升高,这可能是一种抑制作用,而在精神病的全面爆发阶段,谷氨酸浓度与症状之间的关系不再是简单的线性关系。
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来源期刊
CiteScore
6.80
自引率
2.30%
发文量
51
审稿时长
2 months
期刊介绍: The Journal of Psychiatry & Neuroscience publishes papers at the intersection of psychiatry and neuroscience that advance our understanding of the neural mechanisms involved in the etiology and treatment of psychiatric disorders. This includes studies on patients with psychiatric disorders, healthy humans, and experimental animals as well as studies in vitro. Original research articles, including clinical trials with a mechanistic component, and review papers will be considered.
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