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谷氨酸成像(GluCEST)显示,精神病谱系患者的大脑GluCEST对比度较低。

Glutamate imaging (GluCEST) reveals lower brain GluCEST contrast in patients on the psychosis spectrum.

作者信息

Roalf D R, Nanga R P R, Rupert P E, Hariharan H, Quarmley M, Calkins M E, Dress E, Prabhakaran K, Elliott M A, Moberg P J, Gur R C, Gur R E, Reddy R, Turetsky B I

机构信息

Neuropsychiatry Section, Department of Psychiatry, Brain Behavior Laboratory, University of Pennsylvania Perelman School of Medicine, University of Pennsylvania, Philadelphia, PA, USA.

Department of Radiology &Center for Magnetic and Optical Imaging, University of Pennsylvania Perelman School of Medicine, University of Pennsylvania, Philadelphia, PA, USA.

出版信息

Mol Psychiatry. 2017 Sep;22(9):1298-1305. doi: 10.1038/mp.2016.258. Epub 2017 Jan 24.

Abstract

Psychosis commonly develops in adolescence or early adulthood. Youths at clinical high risk (CHR) for psychosis exhibit similar, subtle symptoms to those with schizophrenia (SZ). Malfunctioning neurotransmitter systems, such as glutamate, are implicated in the disease progression of psychosis. Yet, in vivo imaging techniques for measuring glutamate across the cortex are limited. Here, we use a novel 7 Tesla MRI glutamate imaging technique (GluCEST) to estimate changes in glutamate levels across cortical and subcortical regions in young healthy individuals and ones on the psychosis spectrum. Individuals on the psychosis spectrum (PS; n=19) and healthy young individuals (HC; n=17) underwent MRI imaging at 3 and 7 T. At 7 T, a single slice GluCEST technique was used to estimate in vivo glutamate. GluCEST contrast was compared within and across the subcortex, frontal, parietal and occipital lobes. Subcortical (χ (1)=4.65, P=0.031) and lobular (χ (1)=5.17, P=0.023) GluCEST contrast levels were lower in PS compared with HC. Abnormal GluCEST contrast levels were evident in both CHR (n=14) and SZ (n=5) subjects, and correlated differentially, across regions, with clinical symptoms. Our findings describe a pattern of abnormal brain neurochemistry early in the course of psychosis. Specifically, CHR and young SZ exhibit diffuse abnormalities in GluCEST contrast attributable to a major contribution from glutamate. We suggest that neurochemical profiles of GluCEST contrast across cortex and subcortex may be considered markers of early psychosis. GluCEST methodology thus shows promise to further elucidate the progression of the psychosis disease state.

摘要

精神病通常在青春期或成年早期发病。处于临床高危(CHR)的青年精神病患者表现出与精神分裂症(SZ)患者相似的细微症状。神经递质系统功能失调,如谷氨酸,与精神病的疾病进展有关。然而,用于测量整个皮层谷氨酸水平的体内成像技术有限。在这里,我们使用一种新型的7特斯拉磁共振成像谷氨酸成像技术(GluCEST)来估计年轻健康个体和精神病谱系个体的皮层和皮层下区域谷氨酸水平的变化。精神病谱系个体(PS;n = 19)和健康年轻个体(HC;n = 17)在3T和7T下接受磁共振成像。在7T时,使用单切片GluCEST技术来估计体内谷氨酸水平。比较了皮层下、额叶、顶叶和枕叶内和之间的GluCEST对比度。与HC相比,PS的皮层下(χ(1)=4.65,P = 0.031)和小叶(χ(1)=5.17,P = 0.023)GluCEST对比度水平较低。在CHR(n = 14)和SZ(n = 5)受试者中均明显存在异常的GluCEST对比度水平,并且在不同区域与临床症状存在差异相关性。我们的研究结果描述了精神病病程早期大脑神经化学异常的一种模式。具体而言,CHR和年轻SZ患者在GluCEST对比度上表现出弥漫性异常,这主要归因于谷氨酸的作用。我们认为,皮层和皮层下GluCEST对比度的神经化学特征可能被视为早期精神病的标志物。因此,GluCEST方法有望进一步阐明精神病疾病状态的进展。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/db0b/5822706/d9d64607d4da/nihms834848f1.jpg

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