Methylation at 3 LCR of HPV16 can be affected by patient age and disruption of E1 or E2 genes
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Virus Research
Abstract
CpG methylation at early promoter of HPV16 DNA, in the 3 end of the Long Control Region (3
LCR), has
been associated to the presence of episomal forms of viral genome and, consequently, intact E1 and E2
ORFs. The DNA methylation would block the access of E2 viral protein to the E2 binding sites at early promoter. However, is still unclear if methylation at 3
LCR of HPV16 DNA can also vary depending of
other tumor characteristics in addition to viral DNA physical state. In this study, we evaluate whether the
methylation level at the five CpG located at 3
LCR of HPV16 is associated to patient age and E1 and/or E2
ORFs integrity. DNA pyrosequencing was used to measure the methylation level in 69 invasive cervical
cancer samples obtained from biopsies of patients attended at Brazilian National Institute of Cancer
(INCA). PCR amplifications were performed to assess disruption status of E1 and E2 genes of HPV16. The
methylation average per sample ranged widely, from <1 to 88.00%. Presence of intact E1/E2 genes and
patient age were positively associated with average methylation in both bivariate analyses (p = 0.003
and p = 0.006, respectively), and multivariate analysis (p = 0.002 and p = 0.021, respectively), adjusted for
tumor type (squamous cell carcinomas or adenocarcinomas) and HPV16 lineage. These findings showed
that presence of intact E1/E2 open reading frames was associated with high levels of DNA methylation,
and older patients showed higher levels of methylation than younger ones independently of viral genome
disruption.