Equivalent DNA methylation variation between monozygotic co-twins and unrelated individuals reveals universal epigenetic inter-individual dissimilarity

Benjamin Planterose Jiménez; Fan Liu; Amke Caliebe; Diego Montiel González; Jordana T. Bell; Manfred Kayser; Athina Vidaki

doi:10.1186/s13059-020-02223-9

Genome Biology (Jan 2021)

Equivalent DNA methylation variation between monozygotic co-twins and unrelated individuals reveals universal epigenetic inter-individual dissimilarity

Benjamin Planterose Jiménez,
Fan Liu,
Amke Caliebe,
Diego Montiel González,
Jordana T. Bell,
Manfred Kayser,
Athina Vidaki

Affiliations

Benjamin Planterose Jiménez: Department of Genetic Identification, Erasmus MC University Medical Center Rotterdam
Fan Liu: Department of Genetic Identification, Erasmus MC University Medical Center Rotterdam
Amke Caliebe: Institute of Medical Informatics and Statistics, Kiel University
Diego Montiel González: Department of Genetic Identification, Erasmus MC University Medical Center Rotterdam
Jordana T. Bell: Department of Twin Research and Genetic Epidemiology, King’s College London
Manfred Kayser: Department of Genetic Identification, Erasmus MC University Medical Center Rotterdam
Athina Vidaki: Department of Genetic Identification, Erasmus MC University Medical Center Rotterdam

DOI: https://doi.org/10.1186/s13059-020-02223-9
Journal volume & issue: Vol. 22, no. 1
pp. 1 – 23

Abstract

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Abstract Background Although the genomes of monozygotic twins are practically identical, their methylomes may evolve divergently throughout their lifetime as a consequence of factors such as the environment or aging. Particularly for young and healthy monozygotic twins, DNA methylation divergence, if any, may be restricted to stochastic processes occurring post-twinning during embryonic development and early life. However, to what extent such stochastic mechanisms can systematically provide a stable source of inter-individual epigenetic variation remains uncertain until now. Results We enriched for inter-individual stochastic variation by using an equivalence testing-based statistical approach on whole blood methylation microarray data from healthy adolescent monozygotic twins. As a result, we identified 333 CpGs displaying similarly large methylation variation between monozygotic co-twins and unrelated individuals. Although their methylation variation surpasses measurement error and is stable in a short timescale, susceptibility to aging is apparent in the long term. Additionally, 46% of these CpGs were replicated in adipose tissue. The identified sites are significantly enriched at the clustered protocadherin loci, known for stochastic methylation in developing neurons. We also confirmed an enrichment in monozygotic twin DNA methylation discordance at these loci in whole genome bisulfite sequencing data from blood and adipose tissue. Conclusions We have isolated a component of stochastic methylation variation, distinct from genetic influence, measurement error, and epigenetic drift. Biomarkers enriched in this component may serve in the future as the basis for universal epigenetic fingerprinting, relevant for instance in the discrimination of monozygotic twin individuals in forensic applications, currently impossible with standard DNA profiling.

Published in Genome Biology

ISSN: 1474-760X (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Science: Biology (General): Genetics
Website: https://genomebiology.biomedcentral.com/

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