FAN Zhengqin, CAO Lingzhi, ZHAO Yun, QUAN Wen, SUN Zhengsong. Analysis in risk factors and gene mutation model of HBV polymerase region in patients with chronic hepatitis B after nucleoside analogues therapy[J]. Journal of Clinical Medicine in Practice, 2017, (5): 54-56. DOI: 10.7619/jcmp.201705015
Citation: FAN Zhengqin, CAO Lingzhi, ZHAO Yun, QUAN Wen, SUN Zhengsong. Analysis in risk factors and gene mutation model of HBV polymerase region in patients with chronic hepatitis B after nucleoside analogues therapy[J]. Journal of Clinical Medicine in Practice, 2017, (5): 54-56. DOI: 10.7619/jcmp.201705015

Analysis in risk factors and gene mutation model of HBV polymerase region in patients with chronic hepatitis B after nucleoside analogues therapy

  • Objective To explore the variation in the gene mutation patterns and risk factors of HBV polymerase region (P) in chronic viral hepatitis (CHB) patients with nucleoside analogues therapy.Methods A total of 108 chronic hepatitis B patients with viral breakthrough after the treatment of nucleoside analogues were selected as the study subjects.The PCR product direct sequencing method was used to analyze the genetic variation of HBV P region.Results Among 108 cases,69 cases were detected by gene drug resistance,and the mutation type amount to 12,among which rtM204I was the most common (30.4%),and the second was rtL180M/rtM204I combined mutation (13%).The proportion of the major nucleoside analogues resistance highest proportion of lamivudine was 62.3%,followed by adefovir dipivoxil (21.7%) and telbivudine (15.9%).There were 33 cases with a single site mutation,29 cases with two sites mutation and 7 cases with three and above sites mutation.In the 7 cases,1 case was treated with lamivudine,1 case with entecavir,and the remaining 5 cases with irregular combined or sequential use of lamivudine,adefovir dipivoxil and entecavir.Conclusion The amino acid of HBV P gene resistant mutation is complex and varied,and rtM204V/I mutation is the most common type.Three and above sites mutation is associated with irregular combined or sequential use of lamivudine,adefovir dipivoxil and entecavir.
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