Risk Of Developing Liver Cancer After HCV Treatment

Friday, March 9, 2018

Role of IL-28B genetic variants in HCV-related liver disease severity in patients with different viral genotypes

Medicine: March 2018 - Volume 97 - Issue 10 - p e9782
Role of IL-28B genetic variants in HCV-related liver disease severity in patients with different viral genotypes
Huang, Ching-I MDa,b; Huang, Chung-Feng MDa,b,c; Yeh, Ming-Lun MDb,c; Lin, Yi-Hung MDb,d; Liang, Po-Cheng MDb,d; Liu, Shang-Yin Vanson PhDe; Hsieh, Meng-Hsuan MDb,c,f; Lin, Zu-Yau MD, PhDb,c; Chen, Shinn-Cherng MD, PhDb,c; Huang, Jee-Fu MD, PhDa,b,c; Chuang, Wan-Long MD, PhDa,b,c; Dai, Chia-Yen MD, PhDa,b,c,f,*; Yu, Ming-Lung MD, PhDa,b,c,*

Full Text
https://journals.lww.com/md-journal/fulltext/2018/03090/Role_of_IL_28B_genetic_variants_in_HCV_related.41.aspx

Abstract
Reports of the role of host interleukin 28B (IL-28B) genetic variants in liver disease severity in patients with chronic hepatitis C (CHC) have obtained conflicting results. The impact of IL-28B in Asian patients with different viral genotypes remains elusive. We try to elucidate the effect of IL-28B genetic variants in a large Asian cohort with different viral genotypes.

The association between the IL-28B rs8099917 genotype and liver fibrosis was investigated in 1288 patients with biopsy-proven CHC. Patients with hepatitis C virus genotype 1 (HCV-1) infection comprised 59.4% of the population. The remaining 40.6% (518 patients) did not have HCV-1 infection. Of the 1084 patients with the IL-28 genotype, 85.6% (928 patients) had the TT genotype. Univariate analysis revealed that, compared to patients without advanced liver fibrosis, patients with advanced liver fibrosis (Metavir fibrosis score 3-4) had an older age, a lower platelet count, a higher α-fetoprotein level, a higher alanine aminotransferase level, a higher incidence of diabetes, and a higher frequency of rs8099917 non-TT genotype carriage.

Logistic regression analysis revealed that factors significantly associated with advanced liver fibrosis included age (odds ratio [OR]/95% confidence interval [CI]: 1.023/1.009-1.037, P = .001), diabetes (OR/CI: 1.736/1.187-2.539, P = .004), α-fetoprotein (OR/CI: 1.007/1.002-1.012, P = .009), platelet count (OR/CI: 0.991/0.988-0.993, P < .001), and carriage of the rs8099917 non-TT genotype (OR/CI: 0.585/0.400-0.856, P = .006).

When patients were classified by viral genotype, factors that had significant independent associations with advanced liver fibrosis in patients with HCV-1 infection included diabetes (OR/CI: 2.379/1.452-3.896, P = .001), α-fetoprotein (OR/CI: 1.023/1.012-1.035, P < .001), platelet count (OR/CI: 0.99/0.987-0.994, P < .001), and carriage of the rs8099917 non-TT genotype (OR/CI: 0.529/0.328-0.854, P = .009).

In patients who had advanced liver fibrosis but not HCV-1 infection, factors that had significant independent associations with advanced liver fibrosis included age (OR/CI: 1.039/1.016-1.063, P = .001) and platelet count (OR/CI: 0.99/0.986-0.995, P < .001); additionally, IL-28B genetic variants were not associated with liver disease severity.

Unfavorable IL-28B genetic variants were associated with advanced liver disease. The genetic effect is limited to patients with HCV-1 infection.

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