Inflammatory Biomarkers, Cognitive Functioning, and Brain Imaging Abnormalities in Bipolar Disorder: A Systematic Review.

IF 2 Q3 CLINICAL NEUROLOGY
Altamura Mario, Leccisotti Ivana, Mollica Anita, Maddalena Silvio, Altamura Claudia, Moretti Mariaclaudia, Bellomo Antonello
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Abstract

Objective: Recent studies have pointed to neuroinflammation and neurotrophic factors as crucial mediators in the pathophysiology origins of mood disorders. The aim of this review is to assess the potential association between cognitive impairment, brain imaging abnormalities, and inflammatory biomarkers in patients affected by bipolar disorder (BD).

Method: Following PRISMA (Preferred Reporting Items for Systematic reviews and Meta-analyses) guidelines, we systematically searched PubMed, Google Scholar, Scopus, and Web of Science databases, with no year restriction, up until August 2023, for human studies that examined the relationship between inflammatory markers and cognitive impairment in BD patients. Studies based on neuroimaging, such as MRI, DTI, and fMRI, were also included, along with those examining the moderating role of specific inflammatory markers in the alteration of the brain.

Results: 59 human clinical studies satisfied the criteria for consideration. Most of the studies reviewed concur that inflammatory state, measured by peripheral blood levels of CRP and cytokines, constitutes an important contributor to cognitive impairment observed in patients with BD. Robust evidence indicates an association between cognitive impairment and CRP, IL-1RA, IL-6, and TNF-α with its receptors, whereas there is no convincing evidence for the involvement of other neuroinflammatory biomarkers. Neuroimaging studies suggest that brain structural/functional abnormalities seen in BD could also be linked to a neuroinflammatory condition.

Conclusions: Current data provide evidence of a link between cognitive impairments observed in BD patients and mechanisms of neuroinflammation. Emerging evidence indicates that systemic inflammation might also play an important role in the deterioration of brain structures critical to cognitive functions in patients with BD. The convergence of findings across these studies strengthens our understanding of the complex neurobiological underpinnings of these disorders. Identification of BD specific inflammatory markers may be of assistance for future early therapeutic interventions.

双相情感障碍的炎症生物标志物、认知功能和脑成像异常:系统回顾
目的:最近的研究指出,神经炎症和神经营养因子是情绪障碍病理生理学起源的关键介质。本综述旨在评估双相情感障碍(BD)患者的认知障碍、脑成像异常和炎症生物标志物之间的潜在关联:根据PRISMA(系统综述和荟萃分析的首选报告项目)指南,我们系统地检索了PubMed、Google Scholar、Scopus和Web of Science数据库(无年份限制,截止到2023年8月)中研究双相情感障碍患者的炎症标志物与认知障碍之间关系的人类研究。此外,还包括基于神经影像学(如 MRI、DTI 和 fMRI)的研究,以及研究特定炎症标志物在大脑变化中的调节作用的研究:59 项人类临床研究符合审议标准。所审查的大多数研究一致认为,以外周血 CRP 和细胞因子水平衡量的炎症状态是导致 BD 患者认知障碍的一个重要因素。大量证据表明,认知障碍与 CRP、IL-1RA、IL-6 和 TNF-α 及其受体有关,但没有令人信服的证据表明其他神经炎症生物标志物也参与其中。神经影像学研究表明,BD 的大脑结构/功能异常也可能与神经炎症有关:目前的数据证明,在 BD 患者中观察到的认知障碍与神经炎症机制之间存在联系。新出现的证据表明,全身性炎症也可能在对 BD 患者认知功能至关重要的大脑结构退化过程中扮演重要角色。这些研究结果的汇集加强了我们对这些疾病复杂的神经生物学基础的了解。鉴定 BD 特异性炎症标志物可能有助于未来的早期治疗干预。
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来源期刊
Clinical Neuropsychiatry
Clinical Neuropsychiatry CLINICAL NEUROLOGY-
CiteScore
11.10
自引率
1.60%
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