| Literature DB >> 33564054 |
Kohei Kashima1,2, Tomoko Kawai3, Riki Nishimura4, Yuh Shiwa5, Kevin Y Urayama6,7, Hiromi Kamura3, Kazue Takeda8, Saki Aoto9, Atsushi Ito4, Keiko Matsubara10, Takeshi Nagamatsu11, Tomoyuki Fujii11, Isaku Omori12, Mitsumasa Shimizu12, Hironobu Hyodo13, Koji Kugu13, Kenji Matsumoto8, Atsushi Shimizu5,14, Akira Oka4, Masashi Mizuguchi15, Kazuhiko Nakabayashi3, Kenichiro Hata3, Naoto Takahashi4.
Abstract
Preterm birth is known to be associated with chronic disease risk in adulthood whereby epigenetic memory may play a mechanistic role in disease susceptibility. Gestational age (GA) is the most important prognostic factor for preterm infants, and numerous DNA methylation alterations associated with GA have been revealed by epigenome-wide association studies. However, in human preterm infants, whether the methylation changes relate to transcription in the fetal state and persist after birth remains to be elucidated. Here, we identified 461 transcripts associated with GA (range 23-41 weeks) and 2093 candidate CpG sites for GA-involved epigenetic memory through analysis of methylome (110 cord blood and 47 postnatal blood) and transcriptional data (55 cord blood). Moreover, we discovered the trends of chromatin state, such as polycomb-binding, among these candidate sites. Fifty-four memory candidate sites showed correlation between methylation and transcription, and the representative corresponding gene was UCN, which encodes urocortin.Entities:
Year: 2021 PMID: 33564054 DOI: 10.1038/s41598-021-83016-3
Source DB: PubMed Journal: Sci Rep ISSN: 2045-2322 Impact factor: 4.379