Plasma miRNAs Correlate with Structural Brain and Cardiac Damage in Friedreich's Ataxia.

IF 2.7 3区 医学 Q3 NEUROSCIENCES Cerebellum Pub Date : 2024-12-17 DOI:10.1007/s12311-024-01766-y
Thiago M Peluzzo, André S Vieira, Alexandre H B Matos, Cynthia Silveira, Mariana Martin, Otávio R C Filho, Thiago J R Rezende, Alberto R M Martinez, Marcondes C França
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Abstract

Friedreich's Ataxia (FRDA) is the most common autosomal recessive ataxia worldwide and is caused by biallelic unstable intronic GAA expansions at FXN. With its limited therapy and the recent approval of the first disease-modifying agent for FRDA, the search for biological markers is urgently needed to assist and ease the development of therapies. MiRNAs have emerged as promising biomarkers in various medical fields such as oncology, cardiology, epilepsy and neurology as well. Cell-free plasmatic miRNAs have potential advantages as biomarkers because of their size, stability against blood RNases, relative ease of obtaining, storage and measurement. In this study, we attempted to characterize the plasma miRNA signature (RNA-Seq followed by qRT-PCR) and its clinical/structural correlates in a cohort of Brazilian patients with FRDA. Our results showed that miR-26a-5p is upregulated and miR-15a-5p is downregulated. The first was correlated with age at onset, cerebellum volume, spinal cord cross-sectional area (C2-CSA) and the left ventricle mass (LV_Mass). For the miR-15a-5p, significant correlations were found with cerebellum volume, spinal cord eccentricity and LV_Mass. It has been previously hypothesized that these miRs target BDNF, modulating its expression and, when this gene is downregulated, it leads to neuronal loss, explaining the ataxic phenotype and our results reinforce this hypothesis. The miR-26a-5p was already associated with cardiomyocyte hypertrophy through the increased NLRP3 inflammasome activity, which is indirectly linked with cardiac hypertrophy. Considering that, we propose these miRNAs as possible prognostic biomarkers for FRDA. However, longitudinal studies are still needed to validate their clinical use.

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血浆mirna与弗里德赖希共济失调的结构性脑和心脏损伤相关。
弗里德雷希共济失调症(FRDA)是全球最常见的常染色体隐性共济失调症,由FXN的双拷贝不稳定内含子GAA扩增引起。由于 FRDA 的治疗方法有限,而且最近批准了第一种改变疾病的药物,因此迫切需要寻找生物标记物来帮助和促进疗法的开发。在肿瘤学、心脏病学、癫痫学和神经学等多个医学领域,miRNA 已成为前景广阔的生物标记物。无细胞浆液 miRNA 具有作为生物标记物的潜在优势,因为它们体积小,对血液 RN 酶稳定,相对容易获得、储存和测量。在这项研究中,我们试图描述巴西一组 FRDA 患者的血浆 miRNA 特征(RNA-Seq,然后是 qRT-PCR)及其临床/结构相关性。结果显示,miR-26a-5p 上调,miR-15a-5p 下调。前者与发病年龄、小脑体积、脊髓横截面积(C2-CSA)和左心室质量(LV_Mass)相关。而 miR-15a-5p 则与小脑体积、脊髓偏心率和左心室质量有显著相关性。以前曾有假设说,这些 miRs 以 BDNF 为靶点,调节其表达,当该基因下调时,会导致神经元缺失,从而解释共济失调表型,我们的研究结果加强了这一假设。miR-26a-5p 已通过增加 NLRP3 炎症小体的活性与心肌细胞肥大有关,而 NLRP3 炎症小体的活性与心肌肥大间接相关。有鉴于此,我们建议将这些 miRNA 作为 FRDA 的可能预后生物标志物。不过,仍需进行纵向研究以验证其临床用途。
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来源期刊
Cerebellum
Cerebellum 医学-神经科学
CiteScore
6.40
自引率
14.30%
发文量
150
审稿时长
4-8 weeks
期刊介绍: Official publication of the Society for Research on the Cerebellum devoted to genetics of cerebellar ataxias, role of cerebellum in motor control and cognitive function, and amid an ageing population, diseases associated with cerebellar dysfunction. The Cerebellum is a central source for the latest developments in fundamental neurosciences including molecular and cellular biology; behavioural neurosciences and neurochemistry; genetics; fundamental and clinical neurophysiology; neurology and neuropathology; cognition and neuroimaging. The Cerebellum benefits neuroscientists in molecular and cellular biology; neurophysiologists; researchers in neurotransmission; neurologists; radiologists; paediatricians; neuropsychologists; students of neurology and psychiatry and others.
期刊最新文献
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