In silico analysis predicts mutational consequences of CITED2, NUDT4, and Ar18B in patients with bipolar disorder

IF 2.6 3区 心理学 Q2 BEHAVIORAL SCIENCES
Harshita Maheshwari, Prekshi Garg, Prachi Srivastava
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引用次数: 0

Abstract

Bipolar disorder is a mood-related disorder, which can be portrayed as extreme shifts in energy, mood, and activity levels which can also be characterized by manic highs and depressive lows that can be often misdiagnosed as unipolar disorder due to primitive diagnostics techniques based on clinical assessments as well as diagnostic complexities arising due to its heterogeneous nature and overlapping symptoms with conditions like schizophrenia. leading to delays in treatment Strong evidence in support of genetic and epigenetic aspects of bipolar disorder, including mechanisms such as compromised hypothalamic-pituitary-adrenal axis, immune-inflammatory imbalances, oxidative stress, and mitochondrial dysfunction are found. Moreover, some previous research has already stated the role of genes like CITED2, NUDT4, and Arl8B in these processes. The primary goal of this study is to investigate the involvement of the genes in exploring and validating their potential as biomarkers for bipolar disorder. In silico tools like MutationTaster, PolyPhen2, SIFT, GTEx, PhenoScanner, and RegulomeDB were used to perform mutational and gene expression analyses. Results revealed potentially dangerous mutations caused in CITED2, NUDT4, and Arl8B, those which can have diverse outcomes. RegulomeDB, GTEx, and PhenoScanner reveal the involvement of these genes in various brain regions highlighting their relevance to bipolar disorder. This analysis suggests the potential utility of CITED2, NUDT4, and Arl8B as diagnostic markers hence shedding light on their roles to elaborate the molecular range of bipolar disorder. The study also contributes to providing valuable insights into the genetic and molecular basis of bipolar disorders.

硅学分析预测双相情感障碍患者中 CITED2、NUDT4 和 Ar18B 的突变后果
双相情感障碍是一种与情绪有关的疾病,表现为精力、情绪和活动水平的极端变化,也可表现为躁狂高涨和抑郁低落,由于基于临床评估的原始诊断技术以及其异质性和与精神分裂症等疾病的重叠症状所导致的诊断复杂性,双相情感障碍常常被误诊为单相情感障碍。双相情感障碍的遗传学和表观遗传学因素,包括下丘脑-垂体-肾上腺轴受损、免疫-炎症失衡、氧化应激和线粒体功能障碍等机制,都是双相情感障碍的有力证据。此外,之前的一些研究已经指出了 CITED2、NUDT4 和 Arl8B 等基因在这些过程中的作用。本研究的主要目的是调查这些基因的参与情况,探索和验证它们作为躁郁症生物标志物的潜力。研究人员使用了 MutationTaster、PolyPhen2、SIFT、GTEx、PhenoScanner 和 RegulomeDB 等硅学工具来进行基因突变和基因表达分析。结果显示,CITED2、NUDT4 和 Arl8B 中的基因突变具有潜在的危险性,这些突变可能会导致不同的结果。RegulomeDB、GTEx和PhenoScanner揭示了这些基因在不同脑区的参与情况,突出了它们与双相情感障碍的相关性。这项分析表明了 CITED2、NUDT4 和 Arl8B 作为诊断标志物的潜在用途,从而揭示了它们在阐明双相情感障碍分子范围方面的作用。这项研究还有助于为双相情感障碍的遗传和分子基础提供有价值的见解。
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来源期刊
Behavioural Brain Research
Behavioural Brain Research 医学-行为科学
CiteScore
5.60
自引率
0.00%
发文量
383
审稿时长
61 days
期刊介绍: Behavioural Brain Research is an international, interdisciplinary journal dedicated to the publication of articles in the field of behavioural neuroscience, broadly defined. Contributions from the entire range of disciplines that comprise the neurosciences, behavioural sciences or cognitive sciences are appropriate, as long as the goal is to delineate the neural mechanisms underlying behaviour. Thus, studies may range from neurophysiological, neuroanatomical, neurochemical or neuropharmacological analysis of brain-behaviour relations, including the use of molecular genetic or behavioural genetic approaches, to studies that involve the use of brain imaging techniques, to neuroethological studies. Reports of original research, of major methodological advances, or of novel conceptual approaches are all encouraged. The journal will also consider critical reviews on selected topics.
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