When the cut-off level of 50% was defined to detect minor populat

When the cut-off level of 50% was defined to detect minor populations by direct sequencing, L31M/V/F mutations and the Y93H mutations were detected in 1.8% (2/110 patients) and 7.3% (8/110) of our patients, respectively, while the values became 1.8% (2/110 patients) and 15.4% (15/110) when 20% was defined as the cut-off level. These results are comparable to the mutation rate determined previously by direct sequencing and that found in the database.[25] Focusing on the Y93H mutation

that is found most frequently in daclatasvir treatment-naïve patients, clinical background factors mTOR inhibitor that would determine efficacy of PEG IFN/RBV combination therapy patients were investigated by univariate analysis of their association with the Y93H substitution (Table 4). Three factors, the IL28B SNP, core a.a. 70 and IRRDR, were found to be correlated with the Y93H substitution with statistical significance in the univariate analysis. In patients with the

Y93H mutation, the major type (TT) was frequently Selinexor observed as the IL28B SNP, while arginine (R) was frequently observed at core a.a. 70 and the number of substitutions in the IRRDR was higher. There was no significant difference in the number of mutations in the ISDR but that number tended to be higher in patients with the Y93H mutation, similar to the IRRDR. The IL28B SNP, core a.a. 70 and IRRDR, which were correlated significantly with the a.a. 93 mutation by univariate analysis, were subjected to multivariate analysis (Table 4). The IL28B SNP major type (TT) was extracted as an independent significant factor with the odds ratio of 3.67 (P = 0.042). The mutation rates of L31M/V/F and

Y93H in each patient, classified 上海皓元 by the IL28 SNP, are presented in Figure 2. Y93H mutations were found significantly more frequently in IL28B TT patients than that in IL28B non-TT patients. In this study, viral mutations conferring resistance to the NS5A replication complex inhibitor daclatasvir were investigated by deep sequencing in daclatasvir treatment-naïve genotype 1b HCV patients and the mutations, especially Y93H, were detected more frequently than predicted by direct sequencing. Interestingly and importantly, the presence of the Y93H mutation correlated with the IL28B SNP of the host, suggesting the possibility that IL28B major type patients who may show a favorable response to IFN have a greater risk of being infected by daclatasvir-resistant HCV.

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