Abstract
Several SNPs located in or around the IL28B gene are associated with response of patients infected with Hepatitis C virus to treatment with pegylated interferon-α +/− ribavirin or with spontaneous clearance of the virus. The results of such studies are so compelling that future treatment approaches are likely to involve clinical decisions being made on the basis of a patient's genotype. Since IL28B is a paralogue of IL28A with greater than 95% sequence identity, it is possible that without genotyping assay specificity, sequences in IL28A may contribute to genotype identification, and potentially confound treatment decisions. This study aimed to 1) examine DNA sequences in IL28B surrounding each of the reported associated SNPs and the corresponding regions in IL28A; and 2) develop a robust assay for rs12979860, the most ‘cosmopolitan’ SNP most strongly associated with treatment response across all global populations studied to date. Bioinformatic analysis of genomic regions surrounding IL28A and IL28B demonstrated that 3 SNPs were unique to IL28B, whereas the remaining 6 SNP regions shared >93% identity between IL28A and IL28B. Using a panel of DNA samples, PCR amplification followed by Sanger sequencing was used to examine IL28B SNPs and the corresponding regions in IL28A. For the overlapping SNPs, all 6 in IL28B were confirmed to be polymorphic whereas the corresponding positions in IL28A were monomorphic. Based upon IL28A and IL28B sequence data, a specific TaqMan® assay was developed for SNP rs12979860 that was 100% concordant to the sequence-derived genotypes. Analysis using a commercial assay identified one discordant result which led to a change in their genotype-calling algorithm. Where future treatment decisions are made upon the results of genotyping assays, it is very important that results are concordant with data from a sequence-based format. This is especially so in situations where designing specific PCR primers is a challenge.
Highlights
Worldwide there are over 170 million individuals who are chronically infected with Hepatitis C virus (HCV) [1]
It was known that sustained virological response (SVR) rates following interferon treatment varied amongst individuals and across different populations suggesting that a genetic component contributed to treatment response
Several single nucleotide polymorphisms (SNPs) located in and around the IL28B gene were found to be associated with treatment response in patients chronically infected with HCV [4,5,6]
Summary
Worldwide there are over 170 million individuals who are chronically infected with Hepatitis C virus (HCV) [1]. Several single nucleotide polymorphisms (SNPs) located in and around the IL28B gene were found to be associated with treatment response in patients chronically infected with HCV [4,5,6]. These papers identified 9 SNPs that were either associated with increased SVR or with a null virological response (NVR). Some of these SNPs were associated with spontaneous clearance of HCV [7] Since these original studies, there have been hundreds of papers examining genotype associations with some of these 9 SNPs. In addition, HCV treatment algorithms that include patient genotype are being considered [8,9]
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