DNA methylation analysis by RRBS of UV irradiated human epidermal melanocytes from neonatal foreskin, HEMn-DP2.
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ABSTRACT: UVR is the greastest risk factor for melanoma develoment. While the role of UVR in DNA mutagenesis is incontrovertable, is is unclear how UVR induced mutations contribute to melanoma. For example, many of the driver mutations ( BRAF V600E or NRAS Q61R) do not bear the UVR signature C>T mutation. To better understand how UVR is contributing to melanoma development, we investigated the non-mutational effect of UVR on the epigenome, specifically DNA methylation. Aberrant DNA methylation changes are a hallmark in melanoma and there are few reports on the effects of UVR ion DNA methylation. We exposed melanocytes to UVR and cultured them for one-month to detect hertible and stable changes in DNA methylation. We found both hyper and hypo methylated sites after UVR exposure. While many of these changes occured outside of promoters and areas of active gene expression, there were changes in promoter DNA methylation changes that correlated with changes in gene expression. These changes also correlated with those found in melanoma and UVR sensitive sites were prognostic of patient overall survival. Our work shows for the first time UVR induced DNA methylation changes in melanocytes and may be another way in which UVR contributes to melanoma development.
ORGANISM(S): Homo sapiens
PROVIDER: GSE169479 | GEO | 2021/04/05
REPOSITORIES: GEO
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