| 拉米夫定耐药株感染者基因型、HBV DNA及多聚酶P区基因变异的关系 |
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| 引用本文: | 卢丹,吕铁锋,章松平,郭晓凤,武静,吴菲,刘斐.拉米夫定耐药株感染者基因型、HBV DNA及多聚酶P区基因变异的关系[J].医学研究杂志,2013,42(12):110-113. |
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| 作者姓名: | 卢丹 吕铁锋 章松平 郭晓凤 武静 吴菲 刘斐 |
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| 作者单位: | [1]浙江中医药大学,杭州310000 [2]杭州市西溪医院,杭州310000 |
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| 摘 要: | 目的分析拉米夫定耐药株感染者的基因型、HBVDNA及多聚酶P区基因变异的关系。方法应用PCR扩增和直接测序法检测83例拉米夫定耐药患者HBV基因型、HBVDNA及多聚酶P区的基因变异。结果83例拉米夫定耐药患者B基因型26例,C基因型57例,B型YIDD变异率69.2%(18/26)、YVDD变异率30.8%(8/26),C型YIDD变异率63.2%(36/57)、YVDD变异率33.3%(19/57),B、c基因型发生YMDD变异模式无统计学差异(P〉0.05);B型rtM204I突变率53.8%(14/26),综合变异率46.2%(12/26),C型rtM2041变异率26.7%(15/57),综合变异率73.7%(42/57),B、C基因型变异位点类型有统计学差异(P〈0.05);耐药变异时c型HBVDNA水平(6.60±1.42)lg拷贝/毫升高于B型(5.88±1.46)1g拷贝/毫升,YIDD变异时c型(6.40±1.48)lg拷贝/毫升、B型(5.68±1.32)1g拷贝/毫升,YVDD变异时C型(6.18±1.87)1g拷贝/毫升、B型(6.82±1.45)lg拷贝/毫升;rtM204I变异时B型(6.12±1.45)lg拷贝/毫升、C型(5.57±1.45)lg拷贝/毫升(P〉0.05);综合变异时c型(6.68±1.51)lg拷贝/毫升,B型(5.76±1.57)lg拷贝/毫升(P〈0.05)。结论c基因型拉米夫定耐药发生率高于B型;基因型与变异位点类型有关,与YMDD变异模式无关;耐药变异时HBVDNA水平c型高于B型,与综合变异有关,与YMDD变异模式无关。
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| 关 键 词: | 乙型肝炎病毒 拉米夫定 病毒载量 基因型 耐药变异 |
Polymerase Region Mutations,Hepatitis B Virus Genotypes and HBV DNA in Chronic Hepatitis B Patients with Lamivudine - resistant HBV Infection |
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| Lu Dan,Lu Tiefeng,Zhang Songping,Guo Xiaofeng,Wufing,Wu Fei,Liu Fei.Polymerase Region Mutations,Hepatitis B Virus Genotypes and HBV DNA in Chronic Hepatitis B Patients with Lamivudine - resistant HBV Infection[J].Journal of Medical Research,2013,42(12):110-113. |
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| Authors: | Lu Dan Lu Tiefeng Zhang Songping Guo Xiaofeng Wufing Wu Fei Liu Fei |
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| Institution: | . Zhefiang Chinese Medical University, Zhefiang 310000, China |
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| Abstract: | Objective To analyze the HBV DNA, mutation patterns of Polymerase region and genotype in patients with lamivudine - resistant HBV infection. Methods Serum samples were collected from 83 hepatitis B patients resistant to lamivudine. HBV P gene was amplified by PCR. The PCR products were detected for the genotypes, polymerase region mutations sites and viral loads directly. Results In 83 cases with 1 amivudine -resistant HBV infection, 26 (31.33% ) were infected with genotype B and 57 (68.67%) with genotype C. 18 patients with HBV genotype B and 36 patients with genotype C developed YIDD mutations (69.2% vs 63.2% ). Meanwhile, 8 pa- tients with genotype B and 19 patients with genotype C developed YVDD mutations (30.8% vs 33.3% ) , therefore, genotype B and C de- veloped YMDD mutations had no significant difference(P 〉0.05). Regard to site mutation, the genotype B developed rtM204I mutation rate(53.8% ) was higher than genotype C (26.7%) and genotype C multi - site mutation rate (73.7%) was higher than genotype B (46.2%) ,and the result was significant difference (P 〈0.05). When HBV have mutated,the levels of HBV DNA in genotype C were higher than those in genotype B (5.88 + 1.46) lg copies/ml vs (6.60 + 1.42) lg eopies/ml, respectively, P 〈 0.05 ) ]. It had no relation to YMDD mutation YIDD mutation (6.40~1.48) vs (5.68 ~l.32),P〉O.05],YVDD mutation(6.82 +1.45) vs (6.18 1.87) , P〉0.051.But it had relation to site mutation(rtM204I mutation (6. 12 1.45) vs (5.57 1.45),P〉0.05],multi-site mutation type C(6.68 +1.51) vs (5.76 +1.57) ,P〈O.051. Conclusion The incidence oflamivudine-resistance in genotype C was higher than in type B. YMDD mutation had no relation to genotypes. Sites mutation was associated with genotypes. The levels of HBV DNA was higher than that in C type. It was related to the multi - site mutation, but had nothing to do with YMDD mutation. |
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| Keywords: | Hepatitis B virus Lamivudine Viral load Genotype Mutation |
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