DNA methylation patterns in the frontal lobe white matter of multiple system atrophy, Parkinson’s disease, and progressive supranuclear palsy: a cross-comparative investigation

IF 9.3 1区 医学 Q1 CLINICAL NEUROLOGY
Megha Murthy, Katherine Fodder, Yasuo Miki, Naiomi Rambarack, Eduardo De Pablo Fernandez, Lasse Pihlstrøm, Jonathan Mill, Thomas T. Warner, Tammaryn Lashley, Conceição Bettencourt
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引用次数: 0

Abstract

Multiple system atrophy (MSA) is a rare neurodegenerative disease characterized by neuronal loss and gliosis, with oligodendroglial cytoplasmic inclusions (GCIs) containing α-synuclein being the primary pathological hallmark. Clinical presentations of MSA overlap with other parkinsonian disorders, such as Parkinson’s disease (PD), dementia with Lewy bodies (DLB), and progressive supranuclear palsy (PSP), posing challenges in early diagnosis. Numerous studies have reported alterations in DNA methylation in neurodegenerative diseases, with candidate loci being identified in various parkinsonian disorders including MSA, PD, and PSP. Although MSA and PSP present with substantial white matter pathology, alterations in white matter have also been reported in PD. However, studies comparing the DNA methylation architectures of white matter in these diseases are lacking. We therefore aimed to investigate genome-wide DNA methylation patterns in the frontal lobe white matter of individuals with MSA (n = 17), PD (n = 17), and PSP (n = 16) along with controls (n = 15) using the Illumina EPIC array, to identify shared and disease-specific DNA methylation alterations. Genome-wide DNA methylation profiling of frontal lobe white matter in the three parkinsonian disorders revealed substantial commonalities in DNA methylation alterations in MSA, PD, and PSP. We further used weighted gene correlation network analysis to identify disease-associated co-methylation signatures and identified dysregulation in processes relating to Wnt signaling, signal transduction, endoplasmic reticulum stress, mitochondrial processes, RNA interference, and endosomal transport to be shared between these parkinsonian disorders. Our overall analysis points toward more similarities in DNA methylation patterns between MSA and PD, both synucleinopathies, compared to that between MSA and PD with PSP, which is a tauopathy. Our results also highlight several shared DNA methylation changes and pathways indicative of converging molecular mechanisms in the white matter contributing toward neurodegeneration in all three parkinsonian disorders.

Abstract Image

多系统萎缩、帕金森病和进行性核上性麻痹额叶白质中的 DNA 甲基化模式:一项交叉比较研究。
多系统萎缩(MSA)是一种罕见的神经退行性疾病,其特征是神经元缺失和神经胶质增生,主要病理特征是含有α-突触核蛋白的少突胶质细胞质包涵体(GCIs)。MSA的临床表现与帕金森病(PD)、路易体痴呆(DLB)和进行性核上性麻痹(PSP)等其他帕金森病重叠,给早期诊断带来了挑战。大量研究报告了神经退行性疾病中 DNA 甲基化的改变,在包括 MSA、PD 和 PSP 在内的各种帕金森病中发现了候选基因位点。虽然多发性硬化症和帕金森病伴有大量白质病变,但帕金森病中也有白质改变的报道。然而,目前还缺乏比较这些疾病中白质 DNA 甲基化结构的研究。因此,我们利用 Illumina EPIC 阵列研究了 MSA(n = 17)、PD(n = 17)和 PSP(n = 16)患者额叶白质以及对照组(n = 15)的全基因组 DNA 甲基化模式,以确定共有的和疾病特异性的 DNA 甲基化改变。对三种帕金森病的额叶白质进行的全基因组DNA甲基化分析表明,MSA、PD和PSP的DNA甲基化改变具有很大的共性。我们进一步使用加权基因相关网络分析来确定与疾病相关的共甲基化特征,并确定了这些帕金森氏病之间共享的 Wnt 信号转导、信号转导、内质网应激、线粒体过程、RNA 干扰和内体转运相关过程的失调。我们的总体分析表明,同为突触核蛋白病的MSA和帕金森病的DNA甲基化模式与同为tau蛋白病的PSP的MSA和帕金森病的DNA甲基化模式相比具有更多的相似性。我们的研究结果还强调了几种共同的DNA甲基化变化和途径,这些变化和途径表明在这三种帕金森病的白质中存在导致神经退行性变的趋同分子机制。
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来源期刊
Acta Neuropathologica
Acta Neuropathologica 医学-病理学
CiteScore
23.70
自引率
3.90%
发文量
118
审稿时长
4-8 weeks
期刊介绍: Acta Neuropathologica publishes top-quality papers on the pathology of neurological diseases and experimental studies on molecular and cellular mechanisms using in vitro and in vivo models, ideally validated by analysis of human tissues. The journal accepts Original Papers, Review Articles, Case Reports, and Scientific Correspondence (Letters). Manuscripts must adhere to ethical standards, including review by appropriate ethics committees for human studies and compliance with principles of laboratory animal care for animal experiments. Failure to comply may result in rejection of the manuscript, and authors are responsible for ensuring accuracy and adherence to these requirements.
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