Numerous mutations in the hepatitis B virus (HBV) genome have been described, but in most cases their role in the pathogenesis of HBV infection is still unclear. Therefore, we analysed specific mutations in HBV-infected Vietnamese patients and assessed their potential relationship with their clinical outcome. A total of 153 HBV-infected Vietnamese patients with well-characterised clinical profiles were enrolled. None of the study participants had a history of alcohol or drug use and none received any antiviral or immunosuppressive therapy before or during the course of this study. The HBx- and core promoter regions were analysed by sequencing. The majority of isolates corresponded to genotype A. The presence of hepatitis B e antigen (HBeAg) was associated with significantly higher viral loads in the chronic HBV-infection group (P = 0.026). Double mutations in the core promoter (1762/1764) were more frequent in those with cancer than in noncancer patients (P < 0.01). Mutations at nucleotide (nt) 1766/1773 were found at low prevalence but with no obvious association to clinical presentation. Cytosine at nt 1858 was predominant but the stop codon mutation in the precore region was not detected. In the study, 4/48 hepatocellular carcinoma (HCC) patients revealed truncated HBx, whilst the serine to alanine mutation (codon 31) of HBx was more prevalent in cancer patients than in asymptomatic HBV carriers (P < 0.01). Thus, the low frequency of mutations indicates the relation of the absence of antiviral pressure in this population. The exclusively found prevalence of certain mutations detected in those with HBV-related carcinoma nevertheless indicates a degree of association with disease progression.
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Khyber Med Coll, Pakistan Hlth Res Council PHRC Res Ctr, Peshawar, PakistanKhyber Med Coll, Pakistan Hlth Res Council PHRC Res Ctr, Peshawar, Pakistan
Ahmad, Israr
Ahmad, Kafeel
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Univ Peshawar, Ctr Biotechnol & Microbiol, Peshawar, PakistanKhyber Med Coll, Pakistan Hlth Res Council PHRC Res Ctr, Peshawar, Pakistan
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ICMR Virus Unit, Kolkata 700010, IndiaInst Blood Transfus Med & Immunohematol, Kolkata, India
Biswas, Avik
Chandra, Partha K.
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Tulane Univ, Sch Med, Dept Pathol & Lab Med, New Orleans, LA 70112 USA
ICMR Virus Unit, Kolkata 700010, IndiaInst Blood Transfus Med & Immunohematol, Kolkata, India
Chandra, Partha K.
Datta, Sibnarayan
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ICMR Virus Unit, Kolkata 700010, IndiaInst Blood Transfus Med & Immunohematol, Kolkata, India
Datta, Sibnarayan
Panigrahi, Rajesh
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ICMR Virus Unit, Kolkata 700010, IndiaInst Blood Transfus Med & Immunohematol, Kolkata, India
Panigrahi, Rajesh
Banerjee, Arup
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St Louis Univ, Div Infect Dis & Immunol, St Louis, MO 63104 USA
ICMR Virus Unit, Kolkata 700010, IndiaInst Blood Transfus Med & Immunohematol, Kolkata, India
Banerjee, Arup
Chakrabarti, Shekhar
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Natl Inst Cholera & Enter Dis, Kolkata, IndiaInst Blood Transfus Med & Immunohematol, Kolkata, India
Chakrabarti, Shekhar
Biswas, Kalidas
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Med Coll & Hosp, Kolkata, IndiaInst Blood Transfus Med & Immunohematol, Kolkata, India
Biswas, Kalidas
Patra, Dipak
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Med Coll & Hosp, Kolkata, IndiaInst Blood Transfus Med & Immunohematol, Kolkata, India
Patra, Dipak
Bhattacharya, Prasun
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Inst Blood Transfus Med & Immunohematol, Kolkata, IndiaInst Blood Transfus Med & Immunohematol, Kolkata, India
Bhattacharya, Prasun
Biswas, Kuntal
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Med Coll & Hosp, Kolkata, IndiaInst Blood Transfus Med & Immunohematol, Kolkata, India
Biswas, Kuntal
Chakravarty, Runu
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ICMR Virus Unit, Kolkata 700010, IndiaInst Blood Transfus Med & Immunohematol, Kolkata, India