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

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

Epigenetics is a rapidly developing field focused on deciphering chemical fingerprints that accumulate on human genomes over time. As the nascent idea of precision medicine expands to encompass epigenetic signatures of diagnostic and prognostic relevance, there is a need for methodologies that provi...

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Bibliographic Details
Main Authors: Adam G. Marsh, Matthew Cottrell, Morton Goldman
Format: Article
Language:English
Published: Frontiers Media S.A. 2016-11-01
Series:Frontiers in Genetics
Subjects:
Blood
DNA Methylation
Lymphocytes
epigenetics
Parkinson's disease
diagnostics
Online Access:http://journal.frontiersin.org/Journal/10.3389/fgene.2016.00191/full
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spelling doaj-6df3c81a386048b28a45ffee8f7514922020-11-24T20:42:24ZengFrontiers Media S.A.Frontiers in Genetics1664-80212016-11-01710.3389/fgene.2016.00191208732Epigenetic DNA Methylation Profiling with MSRE: A Quantitative NGS Approach Using a Parkinson's Disease Test CaseAdam G. Marsh0Adam G. Marsh1Matthew Cottrell2Matthew Cottrell3Morton Goldman4University of DelawareGenome Profiling LLCGenome Profiling LLCUniversity of DelawareGenome Profiling LLCEpigenetics is a rapidly developing field focused on deciphering chemical fingerprints that accumulate on human genomes over time. As the nascent idea of precision medicine expands to encompass epigenetic signatures of diagnostic and prognostic relevance, there is a need for methodologies that provide high-throughput DNA methylation profiling measurements. Here we report a novel quantification methodology for computationally reconstructing site-specific CpG methylation status from next generation sequencing (NGS) data using methyl-sensitive restriction endonucleases (MSRE). An integrated pipeline efficiently incorporates raw NGS metrics into a statistical discrimination platform to identify functional linkages between shifts in epigenetic DNA methylation and disease phenotypes in samples being analyzed. In this pilot proof-of-concept study we quantify and compare DNA methylation in blood serum of individuals with Parkinson's Disease relative to matched healthy blood profiles. Even with a small study of only six samples, a high degree of statistical discrimination was achieved based on CpG methylation profiles between groups, with 1,008 statistically different CpG sites (p textless 0.0025, after false discovery rate correction). A methylation load calculation was used to assess higher order impacts of methylation shifts on genes and pathways and most notably identified FGF3, FGF8, HTT, KMTA5, MIR8073, and YWHAG as differentially methylated genes with high relevance to Parkinson's Disease and neurodegeneration (based on PubMed literature citations). Of these, KMTA5 is a histone methyl-transferase gene and HTT is Huntington Disease Protein or Huntingtin, for which there are well established neurodegenerative impacts. The future need for precision diagnostics now requires more tools for exploring epigenetic processes that may be linked to cellular dysfunction and subsequent disease progression.http://journal.frontiersin.org/Journal/10.3389/fgene.2016.00191/fullBloodDNA MethylationLymphocytesepigeneticsParkinson's diseasediagnostics
collection DOAJ
language English
format Article
sources DOAJ
author Adam G. Marsh
Adam G. Marsh
Matthew Cottrell
Matthew Cottrell
Morton Goldman
spellingShingle Adam G. Marsh
Adam G. Marsh
Matthew Cottrell
Matthew Cottrell
Morton Goldman
Epigenetic DNA Methylation Profiling with MSRE: A Quantitative NGS Approach Using a Parkinson's Disease Test Case
Frontiers in Genetics
Blood
DNA Methylation
Lymphocytes
epigenetics
Parkinson's disease
diagnostics
author_facet Adam G. Marsh
Adam G. Marsh
Matthew Cottrell
Matthew Cottrell
Morton Goldman
author_sort Adam G. Marsh
title Epigenetic DNA Methylation Profiling with MSRE: A Quantitative NGS Approach Using a Parkinson's Disease Test Case
title_short Epigenetic DNA Methylation Profiling with MSRE: A Quantitative NGS Approach Using a Parkinson's Disease Test Case
title_full Epigenetic DNA Methylation Profiling with MSRE: A Quantitative NGS Approach Using a Parkinson's Disease Test Case
title_fullStr Epigenetic DNA Methylation Profiling with MSRE: A Quantitative NGS Approach Using a Parkinson's Disease Test Case
title_full_unstemmed Epigenetic DNA Methylation Profiling with MSRE: A Quantitative NGS Approach Using a Parkinson's Disease Test Case
title_sort epigenetic dna methylation profiling with msre: a quantitative ngs approach using a parkinson's disease test case
publisher Frontiers Media S.A.
series Frontiers in Genetics
issn 1664-8021
publishDate 2016-11-01
description Epigenetics is a rapidly developing field focused on deciphering chemical fingerprints that accumulate on human genomes over time. As the nascent idea of precision medicine expands to encompass epigenetic signatures of diagnostic and prognostic relevance, there is a need for methodologies that provide high-throughput DNA methylation profiling measurements. Here we report a novel quantification methodology for computationally reconstructing site-specific CpG methylation status from next generation sequencing (NGS) data using methyl-sensitive restriction endonucleases (MSRE). An integrated pipeline efficiently incorporates raw NGS metrics into a statistical discrimination platform to identify functional linkages between shifts in epigenetic DNA methylation and disease phenotypes in samples being analyzed. In this pilot proof-of-concept study we quantify and compare DNA methylation in blood serum of individuals with Parkinson's Disease relative to matched healthy blood profiles. Even with a small study of only six samples, a high degree of statistical discrimination was achieved based on CpG methylation profiles between groups, with 1,008 statistically different CpG sites (p textless 0.0025, after false discovery rate correction). A methylation load calculation was used to assess higher order impacts of methylation shifts on genes and pathways and most notably identified FGF3, FGF8, HTT, KMTA5, MIR8073, and YWHAG as differentially methylated genes with high relevance to Parkinson's Disease and neurodegeneration (based on PubMed literature citations). Of these, KMTA5 is a histone methyl-transferase gene and HTT is Huntington Disease Protein or Huntingtin, for which there are well established neurodegenerative impacts. The future need for precision diagnostics now requires more tools for exploring epigenetic processes that may be linked to cellular dysfunction and subsequent disease progression.
topic Blood
DNA Methylation
Lymphocytes
epigenetics
Parkinson's disease
diagnostics
url http://journal.frontiersin.org/Journal/10.3389/fgene.2016.00191/full
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