| Literature DB >> 33504850 |
Hirotaka Yamagata1,2, Hiroyuki Ogihara3, Koji Matsuo4,5, Shusaku Uchida4,6,7, Ayumi Kobayashi4, Tomoe Seki4,6, Masaaki Kobayashi4, Kenichiro Harada4, Chong Chen4, Shigeo Miyata8,9, Masato Fukuda9, Masahiko Mikuni9,10,11, Yoshihiko Hamamoto3, Yoshifumi Watanabe4,12, Shin Nakagawa4.
Abstract
The heterogeneity of major depressive disorder (MDD) is attributed to the fact that diagnostic criteria (e.g., DSM-5) are only based on clinical symptoms. The discovery of blood biomarkers has the potential to change the diagnosis of MDD. The purpose of this study was to identify blood biomarkers of DNA methylation by strategically subtyping patients with MDD by onset age. We analyzed genome-wide DNA methylation of patients with adult-onset depression (AOD; age ≥ 50 years, age at depression onset < 50 years; N = 10) and late-onset depression (LOD; age ≥ 50 years, age at depression onset ≥ 50 years; N = 25) in comparison to that of 30 healthy subjects. The methylation profile of the AOD group was not only different from that of the LOD group but also more homogenous. Six identified methylation CpG sites were validated by pyrosequencing and amplicon bisulfite sequencing as potential markers for AOD in a second set of independent patients with AOD and healthy control subjects (N = 11). The combination of three specific methylation markers achieved the highest accuracy (sensitivity, 64%; specificity, 91%; accuracy, 77%). Taken together, our findings suggest that DNA methylation markers are more suitable for AOD than for LOD patients.Entities:
Year: 2021 PMID: 33504850 PMCID: PMC7840753 DOI: 10.1038/s41598-021-81758-8
Source DB: PubMed Journal: Sci Rep ISSN: 2045-2322 Impact factor: 4.379