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阐明双相情感障碍和精神分裂症早期错配负波缺陷的谷氨酸能过程:一项 H-MRS 和 EEG 联合研究。

Elucidating the glutamatergic processes underlying mismatch negativity deficits in early stage bipolar disorder and schizophrenia: A combined H-MRS and EEG study.

机构信息

Monash Alfred Psychiatry Research Centre, The Alfred and the Central Clinical School, Monash University, Australia; Brain and Mind Centre, University of Sydney, Australia.

Translational Australian Clinical Toxicology (TACT) Research Group, Discipline of Pharmacology, Sydney Medical School, University of Sydney, NSW, Australia.

出版信息

J Psychiatr Res. 2019 Jun;113:83-89. doi: 10.1016/j.jpsychires.2019.03.018. Epub 2019 Mar 24.

Abstract

Impairments in mismatch negativity (MMN) in schizophrenia are well-established; these findings have been extended to show impairments at early illness stages and in bipolar disorder. A substantial literature supports MMN as an index of NMDA receptor output, however, few studies have conducted in vivo assessments to elucidate the neurochemical underpinnings of MMN. Sixty young (16-33 years) participants with bipolar disorder (n = 47) or schizophrenia (n = 13) underwent H-MRS and MMN assessment. Glutamate over creatine (Glu/Cr) levels in the anterior cingulate cortex (ACC) and hippocampus were determined and MMN was measured frontally and temporally. Correlational analyses assessed the relationship between MMN amplitudes and Glu/Cr. Any significant relationships were assessed for specificity with a follow up correlation analysis of MMN and n-acetyleaspartate (NAA/Cr). No associations between frontal or temporal MMN and ACC or hippocampal Glu/Cr were noted in the bipolar group. In the schizophrenia group, frontal and right temporal MMN amplitudes corresponded with increased ACC Glu/Cr at the trend-level. Right temporal MMN was similarly significantly associated with NAA/Cr. MMN was not associated with hippocampal Glu/Cr. This work provides in vivo evidence that glutamatergic processes may underlie MMN generation in early stage schizophrenia but not in early stage bipolar disorder suggesting differences in the MMN mechanism in these groups. The negative association between ACC Glu/Cr and MMN is consistent with findings of reduced MMN and increased in vivo glutamatergic neurometabolite levels in early stage schizophrenia. Furthermore, these results indicate that examining in vivo NAA/Cr may have provide additional insights into the MMN mechanism in schizophrenia.

摘要

精神分裂症患者的失匹配负波(MMN)损伤是公认的;这些发现已经扩展到表明在疾病早期阶段和双相情感障碍中存在损伤。大量文献支持 MMN 作为 NMDA 受体输出的指标,然而,很少有研究进行体内评估来阐明 MMN 的神经化学基础。60 名年轻(16-33 岁)的双相情感障碍(n=47)或精神分裂症(n=13)患者接受了 H-MRS 和 MMN 评估。在前扣带皮层(ACC)和海马体中测定谷氨酸与肌酸的比值(Glu/Cr)水平,并在额部和颞部测量 MMN。相关分析评估了 MMN 振幅与 Glu/Cr 之间的关系。如果存在显著的相关性,则通过对 MMN 和 N-乙酰天门冬氨酸(NAA/Cr)的后续相关性分析来评估其特异性。在双相组中,额部或颞部 MMN 与 ACC 或海马体的 Glu/Cr 之间没有关联。在精神分裂症组中,额部和右侧颞部 MMN 振幅与 ACC 的 Glu/Cr 呈趋势水平相关。右侧颞部 MMN 也与 NAA/Cr 显著相关。右颞部 MMN 与海马体的 Glu/Cr 无相关性。这项工作提供了体内证据,表明谷氨酸能过程可能是精神分裂症早期阶段 MMN 产生的基础,但不是早期双相情感障碍的基础,这表明这些群体中 MMN 机制的差异。ACC 的 Glu/Cr 与 MMN 之间的负相关与早期精神分裂症中 MMN 减少和体内谷氨酸能神经代谢物水平升高的发现一致。此外,这些结果表明,检查体内 NAA/Cr 可能为精神分裂症的 MMN 机制提供更多见解。

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