Alterations in 5hmC level and genomic distribution in aging-related epigenetic drift in human adipose stem cells

Author:

Borkowska Joanna1ORCID,Domaszewska-Szostek Anna1,Kołodziej Paulina2,Wicik Zofia1,Połosak Jacek1,Buyanovskaya Olga1,Charzewski Lukasz3,Stańczyk Marek4,Noszczyk Bartłomiej5,Puzianowska-Kuznicka Monika12

Affiliation:

1. Department of Human Epigenetics, Mossakowski Medical Research Centre, PAS, 5 Pawinskiego Street, 02-106 Warsaw, Poland

2. Department of Geriatrics & Gerontology, Medical Centre of Postgraduate Education, 61/63 Kleczewska Street, 01-826 Warsaw, Poland

3. Faculty of Physics, University of Warsaw, 5 Pasteur Street, 02-093 Warsaw, Poland

4. Department of General Surgery, Wolski Hospital, 17 Kasprzaka Street, 01-211 Warsaw, Poland

5. Department of Plastic Surgery, Medical Centre of Postgraduate Education, 99/103 Marymoncka Street, 01-813 Warsaw, Poland

Abstract

Aim: To clarify mechanisms affecting the level and distribution of 5-hydroxymethylcytosine (5hmC) during aging. Materials & methods: We examined levels and genomic distribution of 5hmC along with the expression of ten–eleven translocation methylcytosine dioxygenases (TETs) in adipose stem cells in young and age-advanced individuals. Results: 5hmC levels were higher in adipose stem cells of age-advanced than young individuals (p = 0.0003), but were not associated with age-related changes in expression of TETs. 5hmC levels correlated with population doubling time (r = 0.62; p = 0.01). We identified 58 differentially hydroxymethylated regions. Hypo-hydroxymethylated differentially hydroxymethylated regions were approximately twofold enriched in CCCTC-binding factor binding sites. Conclusion: Accumulation of 5hmC in aged cells can result from inefficient active demethylation due to altered TETs activity and reduced passive demethylation due to slower proliferation.

Publisher

Future Medicine Ltd

Subject

Cancer Research,Genetics

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