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Hepatitis B Virus Genotypes, Expression Quantitative Trait Loci For ZNRD1-AS1 And Their Interactions In Hepatocellular Carcinoma

Posted on:2017-01-05Degree:MasterType:Thesis
Country:ChinaCandidate:Z Z LiuFull Text:PDF
GTID:2284330485962689Subject:Internal medicine (digestive diseases)
Abstract/Summary:PDF Full Text Request
Genetic variants in zinc ribbon domain-containing 1 antisense RNA 1 (ZNRD1-AS1) have been reported to be associated with development of hepatocellular carcinoma (HCC). We sought to determine the influences of ZNRD1-AS1 polymorphisms and their interactions with Hepatitis B virus (HBV) genotypes on the risk of HCC. In this study, we conducted a large population case-control study with 1,507 HBV-related HCC cases and 1,560 HBV persistent carriers. Three single-nucleotide polymorphisms (SNPs) in ZNRD1-AS1 (rs3757328, rs6940552 and rs9261204) were genotyped using a TaqMan allelic discrimination assay, and the HBV genotypes were identified by multiplex PCR. We found consistently significant associations between the ZNRD1-AS1 rs6940552 and rs9261204 SNPs and an increased risk of HCC (additive genetic model:adjusted OR = 1.16,95%CI= 1.03-1.32 for rs6940552; adjusted OR=1.20,95%CI= 1.06-1.35 for rs9261204) and found a borderline association between rs3757328 and HCC risk. Besides, we observed a dose-dependent relationship between increasing numbers of variant alleles of the SNPs and HCC risk (P for trend <0.001). Moreover, we observed a stronger combined effect of the three SNPs on HCC risk among the subjects infected with non-B genotype HBV (adjusted OR= 1.26,95%CI= 1.05-1.50) compared with HBV B-related genotypes (adjusted OR= 0.89,95%CI= 0.69-1.15; P= 0.029 for heterogeneity test). We also found that a multiplicative interaction between the variant alleles and the HBV genotype significantly affected HCC susceptibility (P= 0.030). Together, these results indicate that ZNRD1-AS1 may influence HCC risk accompanied by HBV genotypes.
Keywords/Search Tags:HCC, susceptibility, eQTL, HBV genotype, interaction
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