Age-associated sperm DNA methylation patterns do not directly persist trans-generationally

Timothy G. Jenkins; Emma R. James; Kenneth I. Aston; Albert Salas-Huetos; Alexander W. Pastuszak; Ken R. Smith; Heidi A. Hanson; James M. Hotaling; Douglas T. Carrell

doi:10.1186/s13072-019-0323-4

Epigenetics & Chromatin (Dec 2019)

Age-associated sperm DNA methylation patterns do not directly persist trans-generationally

Timothy G. Jenkins,
Emma R. James,
Kenneth I. Aston,
Albert Salas-Huetos,
Alexander W. Pastuszak,
Ken R. Smith,
Heidi A. Hanson,
James M. Hotaling,
Douglas T. Carrell

Affiliations

Timothy G. Jenkins: Department of Physiology and Developmental Biology, Brigham Young University Provo
Emma R. James: Andrology and IVF Laboratories, University of Utah School of Medicine
Kenneth I. Aston: Andrology and IVF Laboratories, University of Utah School of Medicine
Albert Salas-Huetos: Andrology and IVF Laboratories, University of Utah School of Medicine
Alexander W. Pastuszak: Department of Surgery (Urology Division), University of Utah School of Medicine
Ken R. Smith: Department of Population Sciences, University of Utah School of Medicine
Heidi A. Hanson: Department of Surgery (Urology Division), University of Utah School of Medicine
James M. Hotaling: Department of Surgery (Urology Division), University of Utah School of Medicine
Douglas T. Carrell: Andrology and IVF Laboratories, University of Utah School of Medicine

DOI: https://doi.org/10.1186/s13072-019-0323-4
Journal volume & issue: Vol. 12, no. 1
pp. 1 – 8

Abstract

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Abstract Background The impact of aging on the sperm methylome is well understood. However, the direct, subsequent impact on offspring and the role of altered sperm DNA methylation alterations in this process remain poorly understood. The well-defined impact of aging on sperm DNA methylation represents an excellent opportunity to trace the direct, transgenerational transmission of these signals. Results We utilized the Illumina MethylationEPIC array to analyze the sperm of 16 patients with older (> 40 years of age) paternal grandfathers (‘old grand paternal age’ patients; OGPA) and 16 patients with younger (< 25 years of age) grandfathers (‘young grand paternal age’ patients; YGPA) identified through the Subfertility Health Assisted Reproduction and the Environment (SHARE) cohort to investigate differences in DNA methylation. No differentially methylated regions were identified between the OGPA and YGPA groups. Further, when assessing only the sites previously shown to be altered by age, no statistically significant differences between OGPA and YGPA were identified. This was true even despite the lower bar for significance after removing multiple comparison correction in a targeted approach. Interestingly though, in an analysis of the 140 loci known to have decreased methylation with age, the majority (~ 72%) had lower methylation in OGPA compared to YGPA though the differences were extremely small (~ 1.5%). Conclusions This study suggests that the robust and consistent age-associated methylation alterations seen in human sperm are ‘reset’ during large-scale epigenetic reprograming processes and are not directly inherited trans-generationally (over two generations). An extremely small trend was present between the YGPA and OGPA groups that resemble the aging pattern in older sperm. However, this trend was not significant and was so small that, if real, is almost certainly biologically inert.

Published in Epigenetics & Chromatin

ISSN: 1756-8935 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Science: Biology (General): Genetics
Website: https://epigeneticsandchromatin.biomedcentral.com/

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