实用肝脏病杂志 ›› 2011, Vol. 14 ›› Issue (1): 25-28.doi: 10.3969/j.issn.1672-5069.2011.01.009

• 论著 • 上一篇    下一篇

拉米夫定耐药致肝衰竭患者病情恶化前后HBV生物学特性变化*

李磊,李宜,高人焘,杨东亮   

  1. 230001 合肥市 安徽医科大学附属省立医院感染病科(李磊,李宜,高人焘);华中科技大学同济医学院附属同济医院临床免疫研究室(杨东亮)
  • 收稿日期:2010-10-08 出版日期:2011-02-10 发布日期:2016-04-15
  • 作者简介:李磊 男,31岁,医学博士,主治医师。主要从事HBV分子病毒学及复制模型研究。E-mail: lilei0403@163.com
  • 基金资助:
    安徽医科大学科研基金资助课题(编号:2010xkj084)

The biological changes of hepatitis B virus in a patient with acute-on-chronic liver failure induced by lamivudine-resistant mutant infection

LI Lei,LI Yi,GAO Rentao,et al.   

  1. Department of Infectious Disease,Anhui Provincial Hospital,Anhui Medical University,Hefei 230001,China
  • Received:2010-10-08 Online:2011-02-10 Published:2016-04-15

摘要: 目的 分析1例拉米夫定耐药变异导致病情恶化患者病毒变异前后HBV生物学特性的变化,为进一步明确YMDD变异生物学意义的相关研究奠定基础。方法 分别构建病情恶化前后含1.3倍HBV基因组的可复制性克隆。体外转染Huh-7细胞系,检测抗原分泌和HBV转录子。使用高压尾静脉注射技术,建立急性感染小鼠模型,比较变异前后毒株病毒血症产生情况。结果 病情恶化前后除HBV YMDD基序发生YVDD变异外,在四个开放读码框内均发生一系列变异。变异前后感染性克隆转染Huh-7细胞72小时HbsAg表达水平无明显变化(P>0.05);变异后病毒HBeAg分泌能力丧失(P<0.01);逆转录PCR半定量检测HBV转录子水平无显著性变化(P>0.05);变异前后感染性克隆建立的HBV急性感染小鼠血清HBV DNA定量分别为7.24±0.63和6.86±0.62lg copies/ml(P>0.05)。结论 该例患者在YMDD变异导致病情恶化前后,除HBeAg分泌功能丧失外,病毒生物学特性无明显变化,提示YMDD基序以外的变异可能具有重要的生物学意义。

关键词: 乙型肝炎病毒, 肝衰竭, 拉米夫定, YMDD

Abstract: Objective To analyze the HBV biological changes pre- and post-clinical exacerbation in an acute-on-chronic liver failure patient caused by HBV YMDD mutation. Methods Two HBV replication competent clones were constructed which contained 1.3 copies of HBV genome and represented the dominant quasispecies before and after clinical exacerbation. Then,they were transfected into Huh-7 cells,and HBsAg and HBeAg in culture supernant were examinanted by ELISA. HBV transcripts in transfected cells was semi-quantified by reverse transcriptional quantified PCR. At the same time,they were employed by hydrodynamic injection into BALB/c mice to establish HBV acute infected model,and the viremia were checked by real-time quantified PCR. Results A series of mutations were observed in all four open reading frames of HBV besides YVDD mutation in YMDD motif after clinical exacerbation. The levels of HBsAg in the supernant of wild and mutant HBV replication competent clones transfected Huh-7 cells were not significantly different(P>0.05),while HbeAg secretion stopped(P<0.01);The HBV transcripts in transfected cells were unchanged(P>0.05);The HBV viremia titer(7.24±0.63 and 6.86±0.62lg copies/ml)were comparable between the two clones(P>0.05). Conclusion There is no significant change in biological characteristics between the HBV clones pre-and post-clinical exacerbation caused by YMDD mutation,except for the defect of HBeAg secretion competence. The mutations locates in the non-reverse transcriptase domain may play some important roles in compensating the viral replication competence.

Key words: Hepatitis B virus, Liver failure, YMDD Mutation