An integrative multi-omics analysis to identify candidate DNA methylation biomarkers related to prostate cancer risk
Wu L; Yang YH; Guo XY; Shu XO; Cai QY; Shu X; Li BS; Tao R; Wu C; Nikas JB; Sun YF; Zhu JJ; Roobol MJ; Giles GG; Brenner H; John EM; Clements J; Grindedal EM; Park JY; Stanford JL; Kote-Jarai Z; Haiman CA; Eeles RA; Zheng W; PRACTICAL consortium; CRUK Consortium; BPC3 Consortium; CAPS Consortium; PEGASUS Consortium
An integrative multi-omics analysis to identify candidate DNA methylation biomarkers related to prostate cancer risk
Wu L
Yang YH
Guo XY
Shu XO
Cai QY
Shu X
Li BS
Tao R
Wu C
Nikas JB
Sun YF
Zhu JJ
Roobol MJ
Giles GG
Brenner H
John EM
Clements J
Grindedal EM
Park JY
Stanford JL
Kote-Jarai Z
Haiman CA
Eeles RA
Zheng W
PRACTICAL consortium
CRUK Consortium
BPC3 Consortium
CAPS Consortium
PEGASUS Consortium
NATURE PUBLISHING GROUP
Julkaisun pysyvä osoite on:
https://urn.fi/URN:NBN:fi-fe2021042821139
https://urn.fi/URN:NBN:fi-fe2021042821139
Tiivistelmä
It remains elusive whether some of the associations identified in genome-wide association studies of prostate cancer (PrCa) may be due to regulatory effects of genetic variants on CpG sites, which may further influence expression of PrCa target genes. To search for CpG sites associated with PrCa risk, here we establish genetic models to predict methylation (N=1,595) and conduct association analyses with PrCa risk (79,194 cases and 61,112 controls). We identify 759 CpG sites showing an association, including 15 located at novel loci. Among those 759 CpG sites, methylation of 42 is associated with expression of 28 adjacent genes. Among 22 genes, 18 show an association with PrCa risk. Overall, 25 CpG sites show consistent association directions for the methylation-gene expression-PrCa pathway. We identify DNA methylation biomarkers associated with PrCa, and our findings suggest that specific CpG sites may influence PrCa via regulating expression of candidate PrCa target genes. Genome wide association studies have identified multiple loci associated with risk of developing prostate cancer but the functional significance of many of these are unknown. Here, after generating models to predict methylation, the authors identify CpG methylation sites associated with prostate cancer.
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