4.6 Article

Nucleotide variants in hepatitis B virus preS region predict the recurrence of hepatocellular carcinoma

Journal

AGING-US
Volume 13, Issue 18, Pages 22256-22275

Publisher

IMPACT JOURNALS LLC

Keywords

hepatitis B virus; viral variant; prediction model; hepatocellular carcinoma; prognosis

Funding

  1. National Natural Science Foundation of China [81520108021, 91529305, 81673250, 81521091, 81373067, 81502882]
  2. State Key Infection Disease Project of China [2017ZX10201201-006-001]
  3. National Key Basic Research Program (973 program) [2015CB554000]

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The study identified HBV preS variants G40C and C147T as serological biomarkers for HCC prognosis, with a prognostic model consisting of serological alpha-fetoprotein and G40C achieving the best performance in predicting postoperative prognosis.
Background: Hepatitis B virus (HBV) variants in the preS region have been associated with hepatocellular carcinoma (HCC). However, the effect of the preS variants on HCC prognosis remains largely unknown. We aimed to identify the preS variants that reliably predict postoperative prognosis in HCC. Methods: RNA-seq data of 203 HCC patients retrieved from public database were screened for the preS variants related to HCC prognosis. The variants in the sera and tumors were then validated in our prospective cohort enrolling 103 HBV-associated HCC patients. Results: By analyzing prognosis-related gene sets in the RNA-seq data, 12 HBV preS variants were associated with HCC recurrence. Of those, G40C and C147T in the sera predicted an unfavorable recurrence-free survival in our cohort (hazard ratio [HR]=2.18, 95% confidence interval [CI]=1.37-3.47, p=0.001 for G40C; HR=1.84, 95% CI=1.15-2.92, p=0.012 for C147T). G40C and C147T were significantly associated with microscopic vascular invasion, larger tumor size, and abnormal liver function. Multivariate Cox regression analysis showed that G40C significantly increased the risk of HCC recurrence in patients with postoperative antiviral treatment. The HCC prognosis-prediction model consisting of alpha-fetoprotein and G40C in the sera achieved the best performance (sensitivity=0.80, specificity=0.70, and area under the curve=0.79). Functional analysis indicated that these two variants were associated with cell proliferation, chromosome instability, carcinogenesis, metastasis, and anticancer drug resistance. Conclusions: G40C and C147T are serological biomarkers for HCC prognosis and the prognostic model consisting of serological alpha-fetoprotein and G40C achieved the best performance in predicting postoperative prognosis.

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