Cargando…
The DNA methylome of human sperm is distinct from blood with little evidence for tissue-consistent obesity associations
Epidemiological research suggests that paternal obesity may increase the risk of fathering small for gestational age offspring. Studies in non-human mammals indicate that such associations could be mediated by DNA methylation changes in spermatozoa that influence offspring development in utero. Huma...
| Autores principales: | , , , , , , , , , |
|---|---|
| Formato: | Online Artículo Texto |
| Lenguaje: | English |
| Publicado: |
Public Library of Science
2020
|
| Materias: | |
| Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7584170/ https://www.ncbi.nlm.nih.gov/pubmed/33048947 http://dx.doi.org/10.1371/journal.pgen.1009035 |
| _version_ | 1783599540911210496 |
|---|---|
| author | Åsenius, Fredrika Gorrie-Stone, Tyler J. Brew, Ama Panchbhaya, Yasmin Williamson, Elizabeth Schalkwyk, Leonard C. Rakyan, Vardhman K. Holland, Michelle L. Marzi, Sarah J. Williams, David J. |
| author_facet | Åsenius, Fredrika Gorrie-Stone, Tyler J. Brew, Ama Panchbhaya, Yasmin Williamson, Elizabeth Schalkwyk, Leonard C. Rakyan, Vardhman K. Holland, Michelle L. Marzi, Sarah J. Williams, David J. |
| author_sort | Åsenius, Fredrika |
| collection | PubMed |
| description | Epidemiological research suggests that paternal obesity may increase the risk of fathering small for gestational age offspring. Studies in non-human mammals indicate that such associations could be mediated by DNA methylation changes in spermatozoa that influence offspring development in utero. Human obesity is associated with differential DNA methylation in peripheral blood. It is unclear, however, whether this differential DNA methylation is reflected in spermatozoa. We profiled genome-wide DNA methylation using the Illumina MethylationEPIC array in a cross-sectional study of matched human blood and sperm from lean (discovery n = 47; replication n = 21) and obese (n = 22) males to analyse tissue covariation of DNA methylation, and identify obesity-associated methylomic signatures. We found that DNA methylation signatures of human blood and spermatozoa are highly discordant, and methylation levels are correlated at only a minority of CpG sites (~1%). At the majority of these sites, DNA methylation appears to be influenced by genetic variation. Obesity-associated DNA methylation in blood was not generally reflected in spermatozoa, and obesity was not associated with altered covariation patterns or accelerated epigenetic ageing in the two tissues. However, one cross-tissue obesity-specific hypermethylated site (cg19357369; chr4:2429884; P = 8.95 × 10(−8); 2% DNA methylation difference) was identified, warranting replication and further investigation. When compared to a wide range of human somatic tissue samples (n = 5,917), spermatozoa displayed differential DNA methylation across pathways enriched in transcriptional regulation. Overall, human sperm displays a unique DNA methylation profile that is highly discordant to, and practically uncorrelated with, that of matched peripheral blood. We observed that obesity was only nominally associated with differential DNA methylation in sperm, and therefore suggest that spermatozoal DNA methylation is an unlikely mediator of intergenerational effects of metabolic traits. |
| format | Online Article Text |
| id | pubmed-7584170 |
| institution | National Center for Biotechnology Information |
| language | English |
| publishDate | 2020 |
| publisher | Public Library of Science |
| record_format | MEDLINE/PubMed |
| spelling | pubmed-75841702020-10-27 The DNA methylome of human sperm is distinct from blood with little evidence for tissue-consistent obesity associations Åsenius, Fredrika Gorrie-Stone, Tyler J. Brew, Ama Panchbhaya, Yasmin Williamson, Elizabeth Schalkwyk, Leonard C. Rakyan, Vardhman K. Holland, Michelle L. Marzi, Sarah J. Williams, David J. PLoS Genet Research Article Epidemiological research suggests that paternal obesity may increase the risk of fathering small for gestational age offspring. Studies in non-human mammals indicate that such associations could be mediated by DNA methylation changes in spermatozoa that influence offspring development in utero. Human obesity is associated with differential DNA methylation in peripheral blood. It is unclear, however, whether this differential DNA methylation is reflected in spermatozoa. We profiled genome-wide DNA methylation using the Illumina MethylationEPIC array in a cross-sectional study of matched human blood and sperm from lean (discovery n = 47; replication n = 21) and obese (n = 22) males to analyse tissue covariation of DNA methylation, and identify obesity-associated methylomic signatures. We found that DNA methylation signatures of human blood and spermatozoa are highly discordant, and methylation levels are correlated at only a minority of CpG sites (~1%). At the majority of these sites, DNA methylation appears to be influenced by genetic variation. Obesity-associated DNA methylation in blood was not generally reflected in spermatozoa, and obesity was not associated with altered covariation patterns or accelerated epigenetic ageing in the two tissues. However, one cross-tissue obesity-specific hypermethylated site (cg19357369; chr4:2429884; P = 8.95 × 10(−8); 2% DNA methylation difference) was identified, warranting replication and further investigation. When compared to a wide range of human somatic tissue samples (n = 5,917), spermatozoa displayed differential DNA methylation across pathways enriched in transcriptional regulation. Overall, human sperm displays a unique DNA methylation profile that is highly discordant to, and practically uncorrelated with, that of matched peripheral blood. We observed that obesity was only nominally associated with differential DNA methylation in sperm, and therefore suggest that spermatozoal DNA methylation is an unlikely mediator of intergenerational effects of metabolic traits. Public Library of Science 2020-10-13 /pmc/articles/PMC7584170/ /pubmed/33048947 http://dx.doi.org/10.1371/journal.pgen.1009035 Text en © 2020 Åsenius et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. |
| spellingShingle | Research Article Åsenius, Fredrika Gorrie-Stone, Tyler J. Brew, Ama Panchbhaya, Yasmin Williamson, Elizabeth Schalkwyk, Leonard C. Rakyan, Vardhman K. Holland, Michelle L. Marzi, Sarah J. Williams, David J. The DNA methylome of human sperm is distinct from blood with little evidence for tissue-consistent obesity associations |
| title | The DNA methylome of human sperm is distinct from blood with little evidence for tissue-consistent obesity associations |
| title_full | The DNA methylome of human sperm is distinct from blood with little evidence for tissue-consistent obesity associations |
| title_fullStr | The DNA methylome of human sperm is distinct from blood with little evidence for tissue-consistent obesity associations |
| title_full_unstemmed | The DNA methylome of human sperm is distinct from blood with little evidence for tissue-consistent obesity associations |
| title_short | The DNA methylome of human sperm is distinct from blood with little evidence for tissue-consistent obesity associations |
| title_sort | dna methylome of human sperm is distinct from blood with little evidence for tissue-consistent obesity associations |
| topic | Research Article |
| url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7584170/ https://www.ncbi.nlm.nih.gov/pubmed/33048947 http://dx.doi.org/10.1371/journal.pgen.1009035 |
| work_keys_str_mv | AT aseniusfredrika thednamethylomeofhumanspermisdistinctfrombloodwithlittleevidencefortissueconsistentobesityassociations AT gorriestonetylerj thednamethylomeofhumanspermisdistinctfrombloodwithlittleevidencefortissueconsistentobesityassociations AT brewama thednamethylomeofhumanspermisdistinctfrombloodwithlittleevidencefortissueconsistentobesityassociations AT panchbhayayasmin thednamethylomeofhumanspermisdistinctfrombloodwithlittleevidencefortissueconsistentobesityassociations AT williamsonelizabeth thednamethylomeofhumanspermisdistinctfrombloodwithlittleevidencefortissueconsistentobesityassociations AT schalkwykleonardc thednamethylomeofhumanspermisdistinctfrombloodwithlittleevidencefortissueconsistentobesityassociations AT rakyanvardhmank thednamethylomeofhumanspermisdistinctfrombloodwithlittleevidencefortissueconsistentobesityassociations AT hollandmichellel thednamethylomeofhumanspermisdistinctfrombloodwithlittleevidencefortissueconsistentobesityassociations AT marzisarahj thednamethylomeofhumanspermisdistinctfrombloodwithlittleevidencefortissueconsistentobesityassociations AT williamsdavidj thednamethylomeofhumanspermisdistinctfrombloodwithlittleevidencefortissueconsistentobesityassociations AT aseniusfredrika dnamethylomeofhumanspermisdistinctfrombloodwithlittleevidencefortissueconsistentobesityassociations AT gorriestonetylerj dnamethylomeofhumanspermisdistinctfrombloodwithlittleevidencefortissueconsistentobesityassociations AT brewama dnamethylomeofhumanspermisdistinctfrombloodwithlittleevidencefortissueconsistentobesityassociations AT panchbhayayasmin dnamethylomeofhumanspermisdistinctfrombloodwithlittleevidencefortissueconsistentobesityassociations AT williamsonelizabeth dnamethylomeofhumanspermisdistinctfrombloodwithlittleevidencefortissueconsistentobesityassociations AT schalkwykleonardc dnamethylomeofhumanspermisdistinctfrombloodwithlittleevidencefortissueconsistentobesityassociations AT rakyanvardhmank dnamethylomeofhumanspermisdistinctfrombloodwithlittleevidencefortissueconsistentobesityassociations AT hollandmichellel dnamethylomeofhumanspermisdistinctfrombloodwithlittleevidencefortissueconsistentobesityassociations AT marzisarahj dnamethylomeofhumanspermisdistinctfrombloodwithlittleevidencefortissueconsistentobesityassociations AT williamsdavidj dnamethylomeofhumanspermisdistinctfrombloodwithlittleevidencefortissueconsistentobesityassociations |