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Hepatitis B virus pre S1 deletion is related to viral replication increase and disease progression 被引量:5

Hepatitis B virus pre S1 deletion is related to viral replication increase and disease progression
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摘要 AIM:To investigate the clinical implications of hepatitis B virus(HBV) pre S1 deletion.METHODS:We developed a fluorescence resonance energy transfer-based real-time polymerase chain reaction(RT-PCR) that can detect four genotypes(wild type, 15-bp, 18-bp and 21-bp deletion).The PCR method was used in two cohorts of Korean chronic HBV subjects with genotype C infections.Cohort Ⅰ included 292 chronic HBV subjects randomly selected from Cheju National University Hospital(Jeju, South Korea) or Seoul National University Hospital(Seoul, South Korea), and cohort Ⅱ included 90 consecutive chronic HBV carriers recruited from Konkuk University Hospital(Seoul, South Korea); the cohort Ⅱ patients did not have hepatocellular carcinoma or liver cirrhosis.RESULTS:The method proposed in this study identified 341 of 382 samples(89.3%).Deletion variants were identified in 100(29.3%) of the 341 detected samples.In both cohorts, the subjects with deletions had a significantly higher Hepatitis B virus e antigen(HBe Ag)-positive seroprevalence [cohort Ⅰ, wild(51.0%) vs deletion(75.0%), P < 0.001; cohort Ⅱ, wild(69.2%) vs deletion(92.9%), P = 0.002] and higher HBV DNA levels [cohort Ⅰ, wild(797.7 pg/m L) vs deletion(1678.9 pg/m L), P = 0.013; cohort Ⅱ, wild(8.3 × 108 copies/m L) vs deletion(2.2 × 109 copies/m L), P = 0.049], compared to subjects with wild type HBV.CONCLUSION:HBV genotype C pre S1 deletion may affect disease progression in chronic HBV subjects through an extended duration of HBe Ag seropositive status and increased HBV replications. AIM:To investigate the clinical implications of hepatitis B virus(HBV) pre S1 deletion.METHODS:We developed a fluorescence resonance energy transfer-based real-time polymerase chain reaction(RT-PCR) that can detect four genotypes(wild type, 15-bp, 18-bp and 21-bp deletion).The PCR method was used in two cohorts of Korean chronic HBV subjects with genotype C infections.Cohort Ⅰ included 292 chronic HBV subjects randomly selected from Cheju National University Hospital(Jeju, South Korea) or Seoul National University Hospital(Seoul, South Korea), and cohort Ⅱ included 90 consecutive chronic HBV carriers recruited from Konkuk University Hospital(Seoul, South Korea); the cohort Ⅱ patients did not have hepatocellular carcinoma or liver cirrhosis.RESULTS:The method proposed in this study identified 341 of 382 samples(89.3%).Deletion variants were identified in 100(29.3%) of the 341 detected samples.In both cohorts, the subjects with deletions had a significantly higher Hepatitis B virus e antigen(HBe Ag)-positive seroprevalence [cohort Ⅰ, wild(51.0%) vs deletion(75.0%), P < 0.001; cohort Ⅱ, wild(69.2%) vs deletion(92.9%), P = 0.002] and higher HBV DNA levels [cohort Ⅰ, wild(797.7 pg/m L) vs deletion(1678.9 pg/m L), P = 0.013; cohort Ⅱ, wild(8.3 × 108 copies/m L) vs deletion(2.2 × 109 copies/m L), P = 0.049], compared to subjects with wild type HBV.CONCLUSION:HBV genotype C pre S1 deletion may affect disease progression in chronic HBV subjects through an extended duration of HBe Ag seropositive status and increased HBV replications.
出处 《World Journal of Gastroenterology》 SCIE CAS 2015年第16期5039-5048,共10页 世界胃肠病学杂志(英文版)
基金 Supported by Grants from National Research Foundation of Korea grant funded by the Korean government(Ministry of Education,Science,and Technology),No.2013-005810 Foundation of Seoul National University Hospital(SNUH research fund),No.0320140140
关键词 HEPATITIS B VIRUS PRES1 start CODON DELETION HEPATITIS B VIRUS e ANTIGEN Hepatocellular carcinoma Genotype C Hepatitis B virus Pre S1 start codon deletion Hepatitis B virus e antigen Hepatocellular carcinoma Genotype C
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同被引文献205

  • 1PatrickArbuthnot,AlexioCapovilla,MichaelKew.Putative role of hepatitis B virus X protein in hepatocarcinogenesis: Effects on apoptosis, DNA repair, mitogen‐activated protein kinase and JAK/STAT pathways[J]. Journal of Gastroenterology and Hepatology . 2001 (4)
  • 2Seoung-Ae Lee,Kijeong Kim,Hong Kim,Bum-Joon Kim.Nucleotide change of codon 182 in the surface gene of hepatitis B virus genotype C leading to truncated surface protein is associated with progression of liver diseases[J].Journal of Hepatology.2011(1)
  • 3Y. M. Park,J. W. Jang,S. H. Yoo,S. H. Kim,I. M. Oh,S. J. Park,Y. S. Jang,S. J. Lee.Combinations of eight key mutations in the X /pre C region and genomic activity of hepatitis B virus are associated with hepatocellular carcinoma[J].J Viral Hepat.2014(3)
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  • 8Ying Xie,Shufeng Liu,Yue Zhao,Zhanjun Guo,Jinsheng Xu.X protein mutations in hepatitis B virus DNA predict postoperative survival in hepatocellular carcinoma[J]. Tumor Biology . 2014 (10)
  • 9Ji Yeon Kim,Eun Hyun Song,Hyun Jung Lee,Yeo Kyoung Oh,Kyung-Hee Choi,Dae-Yeul Yu,Sang Ick Park,Je-Kyung Seong,Won-Ho Kim.HBx-Induced Hepatic Steatosis and Apoptosis Are Regulated by TNFR1- and NF-κB-Dependent Pathways[J]. Journal of Molecular Biology . 2010 (4)
  • 10Dake Zhang,Sufang Ma,Xin Zhang,Hanqing Zhao,Huiguo Ding,Changqing Zeng.Prevalent HBV point mutations and mutation combinations at BCP/preC region and their association with liver disease progression. BMC Infectious Diseases . 2010

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