Novel HBsAg mutations correlate with hepatocellular carcinoma, hamper HBsAg secretion and promote cell proliferation in vitro

نویسندگان

  • Romina Salpini
  • Matteo Surdo
  • Nadia Warner
  • Maria Francesca Cortese
  • Danny Colledge
  • Sally Soppe
  • Maria Concetta Bellocchi
  • Daniele Armenia
  • Luca Carioti
  • Fabio Continenza
  • Domenico Di Carlo
  • Patrizia Saccomandi
  • Carmen Mirabelli
  • Michela Pollicita
  • Roberta Longo
  • Sara Romano
  • Giuseppina Cappiello
  • Alberto Spanò
  • Pascale Trimoulet
  • Herve Fleury
  • Jacopo Vecchiet
  • Nerio Iapadre
  • Angelo Barlattani
  • Ada Bertoli
  • Terenzio Mari
  • Caterina Pasquazzi
  • Gabriele Missale
  • Cesare Sarrecchia
  • Elisa Orecchini
  • Alessandro Michienzi
  • Massimo Andreoni
  • Simona Francioso
  • Mario Angelico
  • Jens Verheyen
  • Francesca Ceccherini-Silberstein
  • Stephen Locarnini
  • Carlo Federico Perno
  • Valentina Svicher
چکیده

BACKGROUND An impaired HBsAg-secretion can increase HBV oncogenic-properties. Here, we investigate genetic-determinants in HBsAg correlated with HBV-induced hepatocellular carcinoma (HCC), and their impact on HBsAg-secretion and cell-proliferation. METHODS This study included 128 chronically HBV-infected patients: 23 with HCC (73.9% D; 26.1% A HBV-genotype), and 105 without cirrhosis/HCC (72.4% D, 27.6% A) as reference-group. The impact of mutations on HBsAg-secretion was assessed by measuring the ratio [secreted/intracellular HBsAg] until day 5 post-transfection. The impact of mutations on cell-cycle advancement was assessed by flow-cytometry. RESULTS Two HBsAg mutations significantly correlated with HCC: P203Q (17.4% [4/23] in HCC vs 1.0% [1/105] in non-HCC, P=0.004); S210R (34.8% [8/23] in HCC vs 3.8% [4/105] in non-HCC, P <0.001); P203Q+S210R (17.4% [4/23] in HCC vs 0% [0/110] in non-HCC, P=0.001). Both mutations reside in trans-membrane C-terminal domain critical for HBsAg-secretion. In in-vitro experiments, P203Q, S210R and P203Q+S210R significantly reduced the ratio [secreted/intracellular HBsAg] compared to wt at each time-point analysed (P <0.05), supporting an impaired HBsAg-secretion. Furthermore, P203Q and P203Q+S210R increased the percentage of cells in S-phase compared to wt, indicating cell-cycle progression (P203Q:26±13%; P203Q+S210R:29±14%; wt:18%±9, P <0.01. Additionally, S210R increased the percentage of cells in G2/M-phase (26±8% for wt versus 33±6% for S210R, P <0.001). CONCLUSIONS Specific mutations in HBsAg C-terminus significantly correlate with HBV-induced HCC. They hamper HBsAg-secretion and are associated with increased cellular proliferation, supporting their involvement in HCC-development. The identification of viral genetic markers associated with HCC is critical to identify patients at higher HCC-risk that may deserve intensive liver monitoring, and/or early anti-HBV therapy.

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عنوان ژورنال:

دوره 8  شماره 

صفحات  -

تاریخ انتشار 2017