Epigenetic DNA Methylation Profiling with MSRE: A Quantitative NGS Approach Using a Parkinson's Disease Test Case

Marsh, Adam G.; Cottrell, Matthew T.; Goldman, Morton F.

doi:10.3389/fgene.2016.00191

Cited by 10 publications

(10 citation statements)

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“…6,7 Several studies have found differential methylation in SNCA and MAPT . 8–11 Furthermore, significant changes in DNA methylation were identified in multiple genes in both blood 10,12,13 and brain. 10 Relevant to the current study, dysregulation of Wnt signaling due to methylation was observed in the frontal cortex and midbrain sections of PD brains.…”

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confidence: 99%

Genome-wide brain DNA methylation analysis suggests epigenetic reprogramming in Parkinson disease

et al. 2019

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ObjectiveGiven the known strong relationship of DNA methylation with environmental exposure, we investigated whether brain regions affected in Parkinson disease (PD) were differentially methylated between PD cases and controls.MethodsDNA chip arrays were used to perform a genome-wide screen of DNA methylation on the dorsal motor nucleus of the vagus (DMV), substantia nigra (SN), and cingulate gyrus (CG) of pathologically confirmed PD cases and controls selected using the criteria of Beecham et al. Analysis examined differentially methylated regions (DMRs) between cases and controls for each brain area. RNA sequencing and pathway analysis were also performed for each brain area.ResultsThirty-eight PD cases and 41 controls were included in the analysis. Methylation studies revealed 234 significant DMR in the DMV, 44 in the SN, and 141 in the CG between cases and controls (Sidak p < 0.05). Pathway analysis of these genes showed significant enrichment for the Wnt signaling pathway (FDR < 0.01).ConclusionsOur data suggest that significant DNA methylation changes exist between cases and controls in PD, especially in the DMV, one of the areas affected earliest in PD. The etiology of these methylation changes is not yet known, but the predominance of methylation changes occurring in the DMV supports the hypothesis that vagus nerve function, perhaps involving the gastrointestinal system, is important in PD pathogenesis. These data also give independent support that genes involved in Wnt signaling are a likely factor in the neurodegenerative processes of PD.

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confidence: 99%

Genome-wide brain DNA methylation analysis suggests epigenetic reprogramming in Parkinson disease

et al. 2019

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“…DNA libraries were prepared from methyl-sensitive restriction endonuclease (MSRE) [ 30 , 31 ] fragmented genomic DNA (gDNA) using HpaII, which recognizes C (CpG) G sites. A standard sequencing protocol was then performed including randomized shearing (Covaris, Woburn, MA) and synthesis of a gDNA fragment library using Illumina TruSeq Nano library synthesis kits (San Diego, CA).…”

Section: Methodsmentioning

confidence: 99%

Epigenetic machine learning: utilizing DNA methylation patterns to predict spastic cerebral palsy

et al. 2018

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BackgroundSpastic cerebral palsy (CP) is a leading cause of physical disability. Most people with spastic CP are born with it, but early diagnosis is challenging, and no current biomarker platform readily identifies affected individuals. The aim of this study was to evaluate epigenetic profiles as biomarkers for spastic CP. A novel analysis pipeline was employed to assess DNA methylation patterns between peripheral blood cells of adolescent subjects (14.9 ± 0.3 years old) with spastic CP and controls at single CpG site resolution.ResultsSignificantly hypo- and hyper-methylated CpG sites associated with spastic CP were identified. Nonmetric multidimensional scaling fully discriminated the CP group from the controls. Machine learning based classification modeling indicated a high potential for a diagnostic model, and 252 sets of 40 or fewer CpG sites achieved near-perfect accuracy within our adolescent cohorts. A pilot test on significantly younger subjects (4.0 ± 1.5 years old) identified subjects with 73% accuracy.ConclusionsAdolescent patients with spastic CP can be distinguished from a non-CP cohort based on DNA methylation patterns in peripheral blood cells. A clinical diagnostic test utilizing a panel of CpG sites may be possible using a simulated classification model. A pilot validation test on patients that were more than 10 years younger than the main adolescent cohorts indicated that distinguishing methylation patterns are present earlier in life. This study is the first to report an epigenetic assay capable of distinguishing a CP cohort.Electronic supplementary materialThe online version of this article (10.1186/s12859-018-2224-0) contains supplementary material, which is available to authorized users.

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“…CpG methylation was calculated using a commercial bioinformatic pipeline to reconstruct probabilities of methylation at CpG sites (as used in Marsh and Pasqualone, 2014; Marsh et al., 2016; Crowgey et al., 2018; Genome Profiling LLC, Newark, DE). An overview of the pipeline workflow is available in Supplementary Figure S1.…”

Section: Methodsmentioning

confidence: 99%

“…Computational reconstruction of CpG methylation is based on a null selection model, where the distribution of m5C modifications at any single CpG site is expected to be 50% in a large population of cells (genome copies) for CpG sites that are non-functional or silent. Where CpG methylation status is important for cellular fitness and thus there is a selection force pushing the m5C distributions away from a 50:50 equilibrium, methylation of those CpG sites among all the cellular genome copies sampled can be measured (Marsh and Pasqualone, 2014; Marsh et al., 2016; Crowgey et al., 2018).…”

Section: Methodsmentioning

confidence: 99%

Cytosine Methylation Within Marine Sediment Microbial Communities: Potential Epigenetic Adaptation to the Environment

2019

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Marine sediments harbor a vast amount of Earth’s microbial biomass, yet little is understood regarding how cells subsist in this low-energy, presumably slow-growth environment. Cells in marine sediments may require additional methods for genetic regulation, such as epigenetic modification via DNA methylation. We investigated this potential phenomenon within a shallow estuary sediment core spanning 100 years of age. Here, we provide evidence of dynamic community m5-cytosine methylation within estuarine sediment metagenomes. The methylation states of individual CpG sites were reconstructed and quantified across three depths within the sediment core. A total of 6,254 CpG sites were aligned for direct comparison of methylation states between samples, and 4,235 of these sites mapped to taxa and genes. Our results demonstrate the presence of differential methylation within environmental CpG sites across an age gradient of sediment. We show that epigenetic modification can be detected via Illumina sequencing within complex environmental communities. The change in methylation state of environmentally relevant genes across depths may indicate a dynamic role of DNA methylation in regulation of biogeochemical processes.

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Epigenetic DNA Methylation Profiling with MSRE: A Quantitative NGS Approach Using a Parkinson's Disease Test Case

Cited by 10 publications

References 57 publications

Genome-wide brain DNA methylation analysis suggests epigenetic reprogramming in Parkinson disease

Genome-wide brain DNA methylation analysis suggests epigenetic reprogramming in Parkinson disease

Epigenetic machine learning: utilizing DNA methylation patterns to predict spastic cerebral palsy

Cytosine Methylation Within Marine Sediment Microbial Communities: Potential Epigenetic Adaptation to the Environment

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