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通过测定接受拉米夫定治疗的慢性乙型肝炎患者的乙肝病毒聚合酶突变来早期检测病毒耐药性。

Early detection of viral resistance by determination of hepatitis B virus polymerase mutations in patients treated by lamivudine for chronic hepatitis B.

作者信息

Nafa S, Ahmed S, Tavan D, Pichoud C, Berby F, Stuyver L, Johnson M, Merle P, Abidi H, Trépo C, Zoulim F

机构信息

Liver Unit, Hôtel Dieu, Place de l'hôpital, Lyon, France.

出版信息

Hepatology. 2000 Nov;32(5):1078-88. doi: 10.1053/jhep.2000.19619.

Abstract

We have analyzed the molecular dynamics of emergence of drug-resistant strains in patients receiving lamivudine therapy for chronic hepatitis B. Twenty consecutive patients with lamivudine resistance were studied (13 hepatitis B e antigen [HBeAg]-positive patients and 7 HBe antibody [anti-HBe]-positive patients). Determination of viral genotype, precore mutants, and polymerase gene mutants (L528M, M552V, M552I) was performed using the research version of Lipa-HBV. Quantitative analysis of HBV DNA was performed using both branched DNA (bDNA) and polymerase chain reaction (PCR) assays. Polymerase mutants (genotypic resistance) were found in 16 of 20 patients. Genotypic resistance was detected earlier than the phenotypic resistance (P =.004). Quantitative PCR allowed detection of viral DNA throughout the entire study period in 16 of 20 patients. Analysis of pretreatment variables showed that high alanine transaminase (ALT) levels (>3 x the upper limit of normal [ULN]) was associated with a more rapid selection of drug-resistant mutants (P =.027) and a high hepatitis B virus (HBV) DNA level (>1,497 Meq/mL, bDNA) with a more rapid occurrence of phenotypic resistance (P =.04). At the time of viral breakthrough, the mean serum HBV-DNA values were not different from the pretreatment values (P =.37). ALT levels were higher in anti-HBe-positive patients compared with pretreatment values and to HBeAg-positive patients (P =.01). In 8 patients, antiviral therapy was modified after viral breakthrough, with the introduction of famciclovir and/or interferon alfa. Viral DNA became undetectable by bDNA in 3 patients who received interferon. Our results suggest that genotypic assays for polymerase mutant detection and quantitative determination of viremia with highly sensitive assay are warranted for an optimal monitoring of antiviral therapy of chronic hepatitis B.

摘要

我们分析了接受拉米夫定治疗的慢性乙型肝炎患者中耐药菌株出现的分子动力学。研究了20例连续出现拉米夫定耐药的患者(13例乙肝e抗原[HBeAg]阳性患者和7例乙肝e抗体[抗-HBe]阳性患者)。使用Lipa-HBV研究版对病毒基因型、前核心突变体和聚合酶基因突变体(L528M、M552V、M552I)进行测定。使用分支DNA(bDNA)和聚合酶链反应(PCR)检测法对HBV DNA进行定量分析。20例患者中有16例发现聚合酶基因突变体(基因型耐药)。基因型耐药比表型耐药更早被检测到(P = 0.004)。定量PCR在整个研究期间能够检测到20例患者中16例的病毒DNA。预处理变量分析显示,高丙氨酸转氨酶(ALT)水平(>正常上限[ULN]的3倍)与耐药突变体的更快选择相关(P = 0.027),而高乙肝病毒(HBV)DNA水平(>1497 Meq/mL,bDNA)与表型耐药的更快出现相关(P = 0.04)。在病毒突破时,血清HBV-DNA的平均数值与预处理值无差异(P = 0.37)。与预处理值相比以及与HBeAg阳性患者相比,抗-HBe阳性患者中的ALT水平更高(P = 0.01)。8例患者在病毒突破后修改了抗病毒治疗方案,加用了泛昔洛韦和/或干扰素α。在接受干扰素治疗的3例患者中,bDNA检测不到病毒DNA。我们的结果表明,采用基因型检测法检测聚合酶基因突变体以及使用高灵敏度检测法定量测定病毒血症,对于慢性乙型肝炎抗病毒治疗的最佳监测是必要的。

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