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Viral genotype and hepatitis B virus DNA levels are correlated with histological liver damage in HBeAg-negative chronic hepatitis B virus infection
by
Sung, Joseph Jao-Yiu
, Tse, Chi-Hang
, Wong, May-Ling
, Leung, Nancy Wai-Yee
, Liew, Chook-Tiew
, Tam, John Siu-Lun
, Chan, Henry Lik-Yuen
, Tsang, Steven Woon-Choi
, Ching, Jessica Yuet-Ling
2002
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Viral genotype and hepatitis B virus DNA levels are correlated with histological liver damage in HBeAg-negative chronic hepatitis B virus infection
by
Sung, Joseph Jao-Yiu
, Tse, Chi-Hang
, Wong, May-Ling
, Leung, Nancy Wai-Yee
, Liew, Chook-Tiew
, Tam, John Siu-Lun
, Chan, Henry Lik-Yuen
, Tsang, Steven Woon-Choi
, Ching, Jessica Yuet-Ling
in
2002
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Viral genotype and hepatitis B virus DNA levels are correlated with histological liver damage in HBeAg-negative chronic hepatitis B virus infection
by
Sung, Joseph Jao-Yiu
, Tse, Chi-Hang
, Wong, May-Ling
, Leung, Nancy Wai-Yee
, Liew, Chook-Tiew
, Tam, John Siu-Lun
, Chan, Henry Lik-Yuen
, Tsang, Steven Woon-Choi
, Ching, Jessica Yuet-Ling
2002
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Viral genotype and hepatitis B virus DNA levels are correlated with histological liver damage in HBeAg-negative chronic hepatitis B virus infection
Journal Article
Viral genotype and hepatitis B virus DNA levels are correlated with histological liver damage in HBeAg-negative chronic hepatitis B virus infection
2002
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Overview
OBJECTIVES:
We aimed to study the relationship between the hepatitis B virus (HBV) genotypes, core promoter/precore stop codon mutations, and histological liver damage among hepatitis B e antigen (HBeAg)-negative patients.
METHODS:
Liver biopsy specimens of 55 HBeAg-negative chronic HBV-infected patients were studied. A histological activity index was scored for degree of necroinflammation (HAI-NI) and fibrosis (HAI-F) as described by Knodell
et al. HBV DNA was determined by a cross-linking assay and polymerase chain reaction (PCR) at the core promoter/precore region and the S region. PCR-positive samples were directly sequenced for core promoter and precore mutations and examined by restriction fragment length polymorphism for genotyping.
RESULTS:
Forty-one males and 14 females at a median age of 43 were studied. HBV DNA was detectable in 32 (58%) and 37 (67%) patients by the cross-linking assay and PCR, respectively, at the time of liver biopsy. The median (range) HAI-NI and HAI-F scores were 5 (1–10) and 2 (0–4), respectively. HBV DNA detectable by either the cross-linking assay or PCR was associated with a higher HAI-NI score. Eleven and 31 patients had genotypes B and C HBV, respectively. Genotype C HBV was associated with higher HAI-NI than genotype B HBV. Core promoter mutations and precore stop codon mutation were detected in 74% and 40% patients, respectively, but they were not associated with higher HAI-NI or HAI-F scores.
CONCLUSIONS:
Detectable HBV DNA and genotype C HBV, but not core promoter or precore stop codon mutations, are associated with more severe liver damage in HBeAg-negative patients.
Publisher
Elsevier Inc
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