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作 者:苏明华[1] 江建宁[1] 周元平[2] 陈茂伟[1] 刘志红[1]
机构地区:[1]广西医科大学第一附属医院感染性疾病科,广西南宁530021 [2]广州南方医院,广东广州510515
出 处:《临床肝胆病杂志》2008年第3期172-174,共3页Journal of Clinical Hepatology
基 金:广西自然科学基金项目(桂科0342009)
摘 要:目的探讨HBV BCP变异与拉米夫定抗病毒治疗后HBVDNA反弹的关系。方法应用PCR-序列分析法,检测拉米夫定治疗(100mg/d)1年以上,达到病毒学应答半年以上,再出现HBV DNA反弹(HBV DNA拷贝数≥1.0×104拷贝/ml)的27例乙型肝炎患者(治疗组),以及19例从未用过抗病毒治疗患者(对照组)的HBV C区基本核心启动子(BCP)的突变位点。结果1.治疗组HBVDNA反弹的27例BCP(A1762T+G1764A)变异检出率44.44%(12/27)高于对照组26.32%(5/19),但无统计学差异,P>0.05。2.4例HBVDNA反弹患者治疗前未检出BCP(A1762T+G1764A)变异,治疗后有2例检出BCP(A1762T+G1764A)变异。结论BCP(T1762/A1764)变异可能与拉米夫定治疗后HBVDNA反弹有关。Objective To investigate the relationship of Hepatitis B virus BCP mutation in the hepatitis B virus (HBV) genome and HBVDNA rebound after with lamivudine therapy. Methods With inspected twenty - seven patients (therapy group, HBVDNA 〉 104 copie4/ml) with HBVDNA rebound after respond to virus beyond 6 months with infecting hepatitis B received ]amivudine (100mg/day) oral application for at least 12 months and nineteen patients( control group) with infecting hepatitis B without treated with the drug of antivirus, we have examined mutation in the Basal Core Promoter(BCP) of the Hepatitis B virus (HBV) of two group by PCR - gene sequence analysis. Results 1. The rate of BCP (A1762T + G1764A) mutations were 44. 44% (12/27) in HBVDNA - negative group beyond control group 6. 32% (5/19), but it has not statistic difference (P 〉0. 05). 2. In the therapy group, BCP(A1762T + G1764A)mutation were not examined in four patients before therapy, but it were examined in two patients after therapy. Conclusion BCP(T1762/A1764)mutation may be associated with HBVDNA rebound after ]amivudine therapy.
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