伴有或不伴有重度抑郁症的创伤后应激障碍患者的内侧前额叶皮层神经递质异常。

IF 2.7 4区 医学 Q2 BIOPHYSICS
NMR in Biomedicine Pub Date : 2024-11-01 Epub Date: 2024-07-25 DOI:10.1002/nbm.5220
Kelley M Swanberg, Hetty Prinsen, Christopher L Averill, Leonardo Campos, Abhinav V Kurada, John H Krystal, Ismene L Petrakis, Lynnette A Averill, Douglas L Rothman, Chadi G Abdallah, Christoph Juchem
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引用次数: 0

摘要

创伤后应激障碍(PTSD)是一种在遭受创伤应激后出现的慢性精神疾病。虽然以前在 4 T 或更低的条件下进行的体内质子(1H)MRS)研究发现了与创伤后应激障碍易感性和/或进展相关的谷氨酸代谢改变,但以前没有在更高的场强下进行过研究。此外,先前的研究也没有广泛探讨重度抑郁障碍(MDD)等精神并发症对创伤后应激障碍相关 1H-MRS 可见脑代谢物异常的影响。在此,我们采用 7 T 1H MRS 检测了伴有 MDD(PTSD+MDD+,N = 6)或不伴有 MDD 的 PTSD 患者内侧前额叶皮层(mPFC)中谷氨酸、谷氨酰胺、GABA 和谷胱甘肽的浓度;N = 6)或无 MDD(PTSD+MDD-;N = 5)的创伤后应激障碍患者,以及无创伤后应激障碍但患有 MDD(PTSD-MDD+;N = 9)或无 MDD(PTSD-MDD-;N = 18)的与创伤不匹配的对照组。与健康的 PTSD-MDD- 对照组相比,患有创伤后应激障碍的参与者 GABA 与谷氨酰胺的比率有所下降,但没有出现单一代谢物异常。然而,当考虑到合并 MDD 时,MDD(而非创伤后应激障碍)诊断与 mPFC 谷氨酰胺浓度升高和谷氨酸:谷氨酰胺比率降低显著相关。此外,所有患有创伤后应激障碍和/或多发性抑郁症的参与者的谷胱甘肽浓度都比患有创伤后应激障碍-多发性抑郁症的健康对照组低。尽管单一代谢物的研究结果有限,但创伤后应激障碍和/或多发性硬化症患者前额叶代谢物浓度的异常模式使监督分类能够将他们与健康对照组区分开来,其敏感性和特异性均达到 80% 以上,其中谷胱甘肽、谷氨酰胺和肌醇一直是分类中最有参考价值的代谢物。我们的研究结果表明,在创伤后应激障碍人群中使用 1H MRS 观察到的 mPFC 谷氨酸代谢异常中,MDD 可能是一个重要因素。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Medial prefrontal cortex neurotransmitter abnormalities in posttraumatic stress disorder with and without comorbidity to major depression.

Posttraumatic stress disorder (PTSD) is a chronic psychiatric condition that follows exposure to a traumatic stressor. Though previous in vivo proton (1H) MRS) research conducted at 4 T or lower has identified alterations in glutamate metabolism associated with PTSD predisposition and/or progression, no prior investigations have been conducted at higher field strength. In addition, earlier studies have not extensively addressed the impact of psychiatric comorbidities such as major depressive disorder (MDD) on PTSD-associated 1H-MRS-visible brain metabolite abnormalities. Here we employ 7 T 1H MRS to examine concentrations of glutamate, glutamine, GABA, and glutathione in the medial prefrontal cortex (mPFC) of PTSD patients with MDD (PTSD+MDD+; N = 6) or without MDD (PTSD+MDD-; N = 5), as well as trauma-unmatched controls without PTSD but with MDD (PTSD-MDD+; N = 9) or without MDD (PTSD-MDD-; N = 18). Participants with PTSD demonstrated decreased ratios of GABA to glutamine relative to healthy PTSD-MDD- controls but no single-metabolite abnormalities. When comorbid MDD was considered, however, MDD but not PTSD diagnosis was significantly associated with increased mPFC glutamine concentration and decreased glutamate:glutamine ratio. In addition, all participants with PTSD and/or MDD collectively demonstrated decreased glutathione relative to healthy PTSD-MDD- controls. Despite limited findings in single metabolites, patterns of abnormality in prefrontal metabolite concentrations among individuals with PTSD and/or MDD enabled supervised classification to separate them from healthy controls with 80+% sensitivity and specificity, with glutathione, glutamine, and myoinositol consistently among the most informative metabolites for this classification. Our findings indicate that MDD can be an important factor in mPFC glutamate metabolism abnormalities observed using 1H MRS in cohorts with PTSD.

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来源期刊
NMR in Biomedicine
NMR in Biomedicine 医学-光谱学
CiteScore
6.00
自引率
10.30%
发文量
209
审稿时长
3-8 weeks
期刊介绍: NMR in Biomedicine is a journal devoted to the publication of original full-length papers, rapid communications and review articles describing the development of magnetic resonance spectroscopy or imaging methods or their use to investigate physiological, biochemical, biophysical or medical problems. Topics for submitted papers should be in one of the following general categories: (a) development of methods and instrumentation for MR of biological systems; (b) studies of normal or diseased organs, tissues or cells; (c) diagnosis or treatment of disease. Reports may cover work on patients or healthy human subjects, in vivo animal experiments, studies of isolated organs or cultured cells, analysis of tissue extracts, NMR theory, experimental techniques, or instrumentation.
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