Poststroke depression (PSD) is the most prevalent psychiatric disorder after stroke, which is independently correlated with negative clinical outcome. The identification of specific biomarkers could help to increase the sensitivity of PSD diagnosis and elucidate its pathophysiological mechanisms. The aim of current study was to review and summarize literature exploring potential biomarkers for PSD diagnosis. The PubMed database was searched for papers published in English from October 1977 to December 2017, 90 of which met inclusion criteria for clinical studies related to PSD biomarkers. PSD biomarkers were subdivided into neuroimaging, molecular, and neurophysiological. Some of them could be recommended to support PSD diagnosing. According to the data, lesions affecting the frontal-subcortical circles of mood regulation (prefrontal cortex, basal nuclei, and thalamus) predominantly in the left hemisphere can be considered as neuroimaging markers and predictors for PSD for at least 1 year after stroke. Additional pontine and lobar cerebral microbleeds in acute stroke patients, as well as severe microvascular lesions of the brain, increase the likelihood of PSD. The following molecular candidates can help to differentiate PSD patients from non-depressed stroke subjects: decreased serum BDNF concentrations; increased early markers of inflammation (high-sensitivity C-reactive protein, ferritin, neopterin, and glutamate), serum pro-inflammatory cytokines (TNF-α, IL-1β, IL-6, IL-18, IFN-γ), as well as pro-inflammatory/anti-inflammatory ratios (TNF-α/IL-10, IL-1β/IL-10, IL-6/IL-10, IL-18/IL-10, IFN-γ/IL-10); lowered complement expression; decreased serum vitamin D levels; hypercortisolemia and blunted cortisol awakening response; S/S 5-HTTLPR, STin2 9/12, and 12/12 genotypes of the serotonin transporter gene SLC6A4, 5-HTR2a 1438 A/A, and BDNF met/met genotypes; higher SLC6A4 promoter and BDNF promoter methylation status. Neurophysiological markers of PSD, that reflect a violation of perception and cognitive processing, are the elongation of the latency of N200, P300, and N400, as well as the decrease in the P300 and N400 amplitude of the event-related potentials. The selected panel of biomarkers may be useful for paraclinical underpinning of PSD diagnosis, clarifying various aspects of its multifactorial pathogenesis, optimizing therapeutic interventions, and assessing treatment effectiveness.
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机译:中风后抑郁症(PSD)是中风后最普遍的精神疾病,与不良的临床结果独立相关。特定生物标志物的鉴定可以帮助提高PSD诊断的敏感性,并阐明其病理生理机制。本研究的目的是回顾和总结探索PSD诊断潜在生物标志物的文献。搜索PubMed数据库以查找1977年10月至2017年12月以英文发表的论文,其中90篇符合PSD生物标志物相关临床研究的纳入标准。 PSD生物标志物细分为神经影像学,分子和神经生理学。可以建议其中一些支持PSD诊断。根据数据,影响卒中后至少一年的主要是左半球影响情绪调节的前皮下皮层环(前额皮层,基底核和丘脑)的病变可被视为PSD的神经影像标志和预测因子。急性中风患者中额外的桥脑和大叶脑微出血以及严重的脑微血管病变,增加了PSD的可能性。以下分子候选物可帮助区分PSD患者和非抑郁中风患者:血清BDNF浓度降低;增加了炎症的早期标志物(高敏C反应蛋白,铁蛋白,新蝶呤和谷氨酸),血清促炎细胞因子(TNF-α,IL-1β,IL-6,IL-18,IFN-γ),以及促炎/抗炎比率(TNF-α/ IL-10,IL-1β/ IL-10,IL-6 / IL-10,IL-18 / IL-10,IFN-γ/ IL-10 );补体表达降低;血清维生素D水平降低;高皮质醇血症和皮质醇唤醒反应迟钝;血清素转运蛋白基因SLC6A4的S / S 5-HTTLPR,STin2 9/12和12/12基因型,5-HTR2a 1438 A / A和BDNF met / met基因型; SLC6A4启动子和BDNF启动子甲基化状态较高。 PSD的神经生理学标志反映了感知和认知过程的违背,是N200,P300和N400潜伏期的延长,以及事件相关电位的P300和N400振幅的减小。所选的生物标志物组可用于PSD诊断的亚临床基础,阐明其多因素发病机制的各个方面,优化治疗干预以及评估治疗效果。
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