| Literature DB >> 30033361 |
Ping Gao1, Ji-Han Xia1, Csilla Sipeky2, Xiao-Ming Dong1, Qin Zhang1, Yuehong Yang1, Peng Zhang3, Sara Pereira Cruz1, Kai Zhang1, Jing Zhu3, Hang-Mao Lee1, Sufyan Suleman1, Nikolaos Giannareas1, Song Liu4, Teuvo L J Tammela5, Anssi Auvinen6, Xiaoyue Wang4, Qilai Huang7, Liguo Wang8, Aki Manninen1, Markku H Vaarala9, Liang Wang3, Johanna Schleutker10, Gong-Hong Wei11.
Abstract
Genome-wide association studies (GWAS) have identified rs11672691 at 19q13 associated with aggressive prostate cancer (PCa). Here, we independently confirmed the finding in a cohort of 2,738 PCa patients and discovered the biological mechanism underlying this association. We found an association of the aggressive PCa-associated allele G of rs11672691 with elevated transcript levels of two biologically plausible candidate genes, PCAT19 and CEACAM21, implicated in PCa cell growth and tumor progression. Mechanistically, rs11672691 resides in an enhancer element and alters the binding site of HOXA2, a novel oncogenic transcription factor with prognostic potential in PCa. Remarkably, CRISPR/Cas9-mediated single-nucleotide editing showed the direct effect of rs11672691 on PCAT19 and CEACAM21 expression and PCa cellular aggressive phenotype. Clinical data demonstrated synergistic effects of rs11672691 genotype and PCAT19/CEACAM21 gene expression on PCa prognosis. These results provide a plausible mechanism for rs11672691 associated with aggressive PCa and thus lay the ground work for translating this finding to the clinic.Entities:
Keywords: CEACAM21; GWAS; HOXA2; PCAT19; aggressive prostate cancer; allele-specific DNA-binding of transcription factor; eQTL; risk stratification; rs11672691; single cell CRISPR/Cas9-mediated editing
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Year: 2018 PMID: 30033361 PMCID: PMC6091222 DOI: 10.1016/j.cell.2018.06.003
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582