Roles of DNA methylation and hydroxymethylation in aging, immunosenescence, and gene regulation 公开

Johnson, Nicholas (Spring 2021)

Permanent URL: https://etd.library.emory.edu/concern/etds/1c18dh005?locale=zh
Published

Abstract

DNA methylation (DNAm) refers to the binding of a methyl group to DNA, which typically occurs at a cytosine nucleotide that is directly followed by a guanine nucleotide from 5’ to 3’. DNAm can hold genes in a stably repressed state. It is associated with age, many chronic diseases and biological processes. DNA hydroxymethylation (DNAhm) is a more recent discovery and less well-characterized than DNAm. Unlike DNAm, DNAhm does not bind to known gene repressors (MBD1, MBD2, MBD3) and is associated with cis-gene expression. I first review the role of DNAm and DNAhm in one such biological process known as immunosenescence. Immunosenescence is the general deterioration of the immune system with age, and it is characterized by functional changes in hematopoietic stem cells (HSCs) and specific blood cell types as well as changes in levels of numerous factors, particularly those involved in inflammation. DNAm and DNAhm is not only associated with many immunosenescence-related processes but both of these epigenetic modifications play a causal role in some of them. In addition to reviewing the role of DNAhm and DNAm in immunosenescence, this dissertation specifically investigates age-related DNAhm and its relationship to age-related gene expression. I observed an overrepresentation of directional consistency between age-related DNAhm and age-related gene expression, which contrasts the repressive gene regulatory role of DNAm. This section is followed by an investigation of the capacity of single-cell methylation sequencing to detect novel imprints. Allele-specific methylation (ASM) is the mechanism underlying the establishment of imprints, which regulate gene expression by holding one allele of a gene in a stably repressed state. In this section, I developed a criteria to detect ASM at the sample-level. I then compared ASM detected at the sample-level to the methylation state in individual cells at CpGs with heterozygous sites sufficiently close to the CpGs to distinguish the methylation state of each allele, which constituted a cellular-level gold-standard. In this comparison, ASM detected in ≥3 samples was also ASM in the cellular-level gold standard 95% of the time. These results demonstrate that single cell methylation sequencing is a powerful tool to detect novel imprints.

TABLE OF CONTENTS

Chapter 1: Introduction p.1

REFERENCES p.6

Chapter 2: The role of DNA methylation and hydroxymethylation on immunosenescence p.11

TABLES p.43

FIGURES p.44

REFERENCES p.47

SUPPLEMENTARY MATERIAL p.60

Chapter 3: Age-related DNA hydroxymethylation is enriched for gene expression and immune system processes in human peripheral blood p.63

TABLES p.84

FIGURES p.86

REFERENCES p.90

SUPPLEMENTARY MATERIAL p.96

Chapter 4: Single cell methylation has the potential to detect novel imprints and distinguish between hemi-methylation and allele-specific methylation

p.125

TABLES p.145

FIGURES p.149

REFERENCES p.156

SUPPLEMENTARY MATERIAL p.158

Chapter 5: Conclusions p.163

About this Dissertation

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Permission granted by the author to include this thesis or dissertation in this repository. All rights reserved by the author. Please contact the author for information regarding the reproduction and use of this thesis or dissertation.

School	Laney Graduate School
Department	Biological and Biomedical Sciences
Subfield / Discipline	Population Biology, Ecology & Evolution
Degree	Ph.D.
Submission	Dissertation
Language	English
Research Field	Biology, Bioinformatics Biology, Genetics Biology, Biostatistics
关键词	epigenetics methylation imprinting aging immunosenescence hydroxymethylation
Committee Chair / Thesis Advisor	Michael Epstein, Emory University David Cutler, Emory University Karen Conneely, Emory University Hao Wu, Emory University Peng Jin, Emory University

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Supplemental Files

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	Supplementary Table 3.3 (Genomic information for the 6,650 DhmRs. Column 1 (binIndex) is a unique index for each of the 6,650 bins, column 2 (chr) indicates the chromosome of the bin, column 3 (start) and 4 (end) are the start and end positions of the bin according to the hg38 build of the human genome, column 5 (featureName) is the name of a genomic feature the bin overlaps, column 6 (featureType) indicates the type of overlapping feature (Gene Body, Promoter, or Enhancer), column 7 is the DESeq2 test statistic and column 8 is the corresponding p-value. DhmRs overlapping multiple genomic features have multiple rows, one for each overlapping feature.)	2021-04-03 17:46:35 -0400	Download
	Supplementary Table 3.4 (Genomic information of the 124 DEGs including the gene name (column 1), the Ensembl name (column 2), chromosome (column 3), start (column 4) and stop position (column 5), DESeq2 test statistic (column 6), p-value (column 7), and q-value)	2021-04-03 17:46:43 -0400	Download

Abstract

Table of Contents

About this Dissertation

Primary PDF

Supplemental Files