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

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-i...

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Autores principales: Salpini, Romina, Surdo, Matteo, Warner, Nadia, Cortese, Maria Francesca, Colledge, Danny, Soppe, Sally, Bellocchi, Maria Concetta, Armenia, Daniele, Carioti, Luca, Continenza, Fabio, Carlo, Domenico Di, Saccomandi, Patrizia, Mirabelli, Carmen, Pollicita, Michela, Longo, Roberta, Romano, Sara, Cappiello, Giuseppina, Spanò, Alberto, Trimoulet, Pascale, Fleury, Herve, Vecchiet, Jacopo, Iapadre, Nerio, Barlattani, Angelo, Bertoli, Ada, Mari, Terenzio, Pasquazzi, Caterina, Missale, Gabriele, Sarrecchia, Cesare, Orecchini, Elisa, Michienzi, Alessandro, Andreoni, Massimo, Francioso, Simona, Angelico, Mario, Verheyen, Jens, Ceccherini-Silberstein, Francesca, Locarnini, Stephen, Perno, Carlo Federico, Svicher, Valentina
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2017
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5362517/
https://www.ncbi.nlm.nih.gov/pubmed/28152517
http://dx.doi.org/10.18632/oncotarget.14944
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author Salpini, Romina
Surdo, Matteo
Warner, Nadia
Cortese, Maria Francesca
Colledge, Danny
Soppe, Sally
Bellocchi, Maria Concetta
Armenia, Daniele
Carioti, Luca
Continenza, Fabio
Carlo, Domenico Di
Saccomandi, Patrizia
Mirabelli, Carmen
Pollicita, Michela
Longo, Roberta
Romano, Sara
Cappiello, Giuseppina
Spanò, Alberto
Trimoulet, Pascale
Fleury, Herve
Vecchiet, Jacopo
Iapadre, Nerio
Barlattani, Angelo
Bertoli, Ada
Mari, Terenzio
Pasquazzi, Caterina
Missale, Gabriele
Sarrecchia, Cesare
Orecchini, Elisa
Michienzi, Alessandro
Andreoni, Massimo
Francioso, Simona
Angelico, Mario
Verheyen, Jens
Ceccherini-Silberstein, Francesca
Locarnini, Stephen
Perno, Carlo Federico
Svicher, Valentina
author_facet Salpini, Romina
Surdo, Matteo
Warner, Nadia
Cortese, Maria Francesca
Colledge, Danny
Soppe, Sally
Bellocchi, Maria Concetta
Armenia, Daniele
Carioti, Luca
Continenza, Fabio
Carlo, Domenico Di
Saccomandi, Patrizia
Mirabelli, Carmen
Pollicita, Michela
Longo, Roberta
Romano, Sara
Cappiello, Giuseppina
Spanò, Alberto
Trimoulet, Pascale
Fleury, Herve
Vecchiet, Jacopo
Iapadre, Nerio
Barlattani, Angelo
Bertoli, Ada
Mari, Terenzio
Pasquazzi, Caterina
Missale, Gabriele
Sarrecchia, Cesare
Orecchini, Elisa
Michienzi, Alessandro
Andreoni, Massimo
Francioso, Simona
Angelico, Mario
Verheyen, Jens
Ceccherini-Silberstein, Francesca
Locarnini, Stephen
Perno, Carlo Federico
Svicher, Valentina
author_sort Salpini, Romina
collection PubMed
description 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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spelling pubmed-53625172017-04-24 Novel HBsAg mutations correlate with hepatocellular carcinoma, hamper HBsAg secretion and promote cell proliferation in vitro Salpini, Romina Surdo, Matteo Warner, Nadia Cortese, Maria Francesca Colledge, Danny Soppe, Sally Bellocchi, Maria Concetta Armenia, Daniele Carioti, Luca Continenza, Fabio Carlo, Domenico Di Saccomandi, Patrizia Mirabelli, Carmen Pollicita, Michela Longo, Roberta Romano, Sara Cappiello, Giuseppina Spanò, Alberto Trimoulet, Pascale Fleury, Herve Vecchiet, Jacopo Iapadre, Nerio Barlattani, Angelo Bertoli, Ada Mari, Terenzio Pasquazzi, Caterina Missale, Gabriele Sarrecchia, Cesare Orecchini, Elisa Michienzi, Alessandro Andreoni, Massimo Francioso, Simona Angelico, Mario Verheyen, Jens Ceccherini-Silberstein, Francesca Locarnini, Stephen Perno, Carlo Federico Svicher, Valentina Oncotarget Research Paper 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. Impact Journals LLC 2017-02-01 /pmc/articles/PMC5362517/ /pubmed/28152517 http://dx.doi.org/10.18632/oncotarget.14944 Text en Copyright: © 2017 Salpini et al. http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Salpini, Romina
Surdo, Matteo
Warner, Nadia
Cortese, Maria Francesca
Colledge, Danny
Soppe, Sally
Bellocchi, Maria Concetta
Armenia, Daniele
Carioti, Luca
Continenza, Fabio
Carlo, Domenico Di
Saccomandi, Patrizia
Mirabelli, Carmen
Pollicita, Michela
Longo, Roberta
Romano, Sara
Cappiello, Giuseppina
Spanò, Alberto
Trimoulet, Pascale
Fleury, Herve
Vecchiet, Jacopo
Iapadre, Nerio
Barlattani, Angelo
Bertoli, Ada
Mari, Terenzio
Pasquazzi, Caterina
Missale, Gabriele
Sarrecchia, Cesare
Orecchini, Elisa
Michienzi, Alessandro
Andreoni, Massimo
Francioso, Simona
Angelico, Mario
Verheyen, Jens
Ceccherini-Silberstein, Francesca
Locarnini, Stephen
Perno, Carlo Federico
Svicher, Valentina
Novel HBsAg mutations correlate with hepatocellular carcinoma, hamper HBsAg secretion and promote cell proliferation in vitro
title Novel HBsAg mutations correlate with hepatocellular carcinoma, hamper HBsAg secretion and promote cell proliferation in vitro
title_full Novel HBsAg mutations correlate with hepatocellular carcinoma, hamper HBsAg secretion and promote cell proliferation in vitro
title_fullStr Novel HBsAg mutations correlate with hepatocellular carcinoma, hamper HBsAg secretion and promote cell proliferation in vitro
title_full_unstemmed Novel HBsAg mutations correlate with hepatocellular carcinoma, hamper HBsAg secretion and promote cell proliferation in vitro
title_short Novel HBsAg mutations correlate with hepatocellular carcinoma, hamper HBsAg secretion and promote cell proliferation in vitro
title_sort novel hbsag mutations correlate with hepatocellular carcinoma, hamper hbsag secretion and promote cell proliferation in vitro
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5362517/
https://www.ncbi.nlm.nih.gov/pubmed/28152517
http://dx.doi.org/10.18632/oncotarget.14944
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