Methylation, Gene Expression, and Risk Genotypes at the TERT‐CLPTM1L Locus in Cervical Cancer

生物 宫颈癌 CpG站点 DNA甲基化 基因型 甲基化 端粒酶 癌症 宫颈上皮内瘤变 基因 癌症研究 发起人 遗传学 基因表达
作者
Dhanya Ramachandran,Qianqian Mao,Dandan Liao,Maud Kamal,Peter Schürmann,Rieke Eisenblätter,Robert Geffers,Bálint Balázs,Lolita Lecompte,Nicolas Servant,Linda Larbi Chérif,Constance Lamy,Sylvain Baulande,Patricia Legoix,Christophe Le Tourneau,Aurélien Latouche,Peter Hillemanns,Suzy Scholl,Thilo Dörk
出处
期刊:Molecular Carcinogenesis [Wiley]
标识
DOI:10.1002/mc.23822
摘要

ABSTRACT The reverse transcriptase subunit of telomerase, TERT, is frequently activated in high‐grade dysplasia and invasive cancers of the uterine cervix. Telomerase activation through hypomethylation of the TERT promoter holds promise as a biomarker for cervical cancer progression, however, specific CpG sites involved in cervical cancer risk remain to be fully defined. A recent genome‐wide association study on cervical cancer identified genetic polymorphisms at 5p13.33 (close to TERT‐CLPTM1L ) but the underlying mechanisms are undetermined. We investigated 529 CpG sites within the TERT promoter region and 3 CpG islands nearby, and 21 CpG sites within CLPTM1L in 190 bisulfite‐converted cervical tumor DNA samples from BioRAIDs (NCT02428842). We identified eight CpG sites within TERT intron 2 where methylation was significantly associated with the genotypes of cervical cancer risk variants rs27070 and rs459961 in cervical tumors after multiple testing correction ( p < 9.4 × 10E−5). Hypermethylation at chr5:1289663 correlated with decreased TERT mRNA levels. In an independent series of 188 normal or dysplastic cervical tissues, rare alleles of rs27070 and rs459961 were associated with low basal CLPTM1L levels and with the absence of TERT mRNA in HPV‐negative samples, consistent with their proposed role as protective variants for cervical cancer. HPV infection was associated with increased CLPTM1L and TERT levels. Collectively, our results provide a link between cervical cancer risk variants, methylation, and gene expression and implicate both TERT and CLPTM1L as genes modulated by genomic background and HPV infection during cervical cancer development.

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