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rtM204Q可能是一种新型的乙肝病毒拉米夫定耐药相关突变。

rtM204Q may serve as a novel lamivudine-resistance-associated mutation of hepatitis B virus.

作者信息

Liu Yan, Xu Zhihui, Wang Yan, Li Xiaodong, Liu Liming, Chen Li, Xin Shaojie, Xu Dongping

机构信息

Institute of Infectious Diseases/Liver Failure Medical Center, Beijing 302 Hospital, Beijing, China.

出版信息

PLoS One. 2014 Feb 24;9(2):e89015. doi: 10.1371/journal.pone.0089015. eCollection 2014.

Abstract

BACKGROUND AND AIMS

Lamivudine (LAM) is still widely used for anti-HBV therapy in China. The study aimed to clarify whether a newly-found rtM204Q mutation from patients was associated with the drug resistance.

METHODS

HBV complete reverse-transcriptase region was screened by direct sequencing and verified by clonal sequencing. Replication-competent plasmids containing patient-derived 1.1mer mutant or wild-type viral genome were constructed and transfected into HepG2 cells. After cultured with or without serially-diluted antiviral drugs, intracellular HBV replicative intermediates were quantitated for calculating the 50% effective concentration of drug (EC₅₀).

RESULTS

A total of 12,000 serum samples of 9,830 patients with chronic HBV infection were screened. rtM204Q mutation was detected in seven LAM-refractory patients. By contrast, rtM204I/rtM204V mutations were detected in 2,502 patients' samples. The rtM204Q emerged either alone or in concomitance with rtM204I/rtM204V, and all were accompanied with virologic breakthrough in clinical course. Clonal sequencing verified that rtM204Q mutant was predominant in viral quasispecies of these samples. Phenotypic analysis showed that rtM204Q mutant had 89.9% of replication capacity and 76-fold increased LAM EC₅₀ of the concomitant wild-type strain. By contrast, rtM204I mutant in the sample had lower replication capacity and higher LAM resistance (46.3% and 1396-fold increased LAM EC₅₀ of the wild-type strain) compared to rtM204Q mutant. rtM204Q mutant was susceptible to adefovir dipivoxil (ADV) in vitro and ADV/ADV+LAM rescue therapy in clinic.

CONCLUSION

rtM204Q is suggested to be a novel LAM-resistance-associated mutation. It conferred a moderate resistance with higher competent natural replication capacity compared to rtM204I mutation.

摘要

背景与目的

在中国,拉米夫定(LAM)仍广泛用于抗乙肝病毒治疗。本研究旨在明确患者中新发现的rtM204Q突变是否与耐药性相关。

方法

通过直接测序筛选乙肝病毒完整逆转录酶区域,并通过克隆测序进行验证。构建含有患者来源的1.1mer突变体或野生型病毒基因组的具有复制能力的质粒,并转染至HepG2细胞。在有或没有系列稀释的抗病毒药物的情况下培养后,对细胞内乙肝病毒复制中间体进行定量,以计算药物的50%有效浓度(EC₅₀)。

结果

共筛选了9830例慢性乙肝病毒感染患者的12000份血清样本。在7例对LAM耐药的患者中检测到rtM204Q突变。相比之下,在2502例患者样本中检测到rtM204I/rtM204V突变。rtM204Q单独出现或与rtM204I/rtM204V同时出现,且在临床病程中均伴有病毒学突破。克隆测序证实rtM204Q突变体在这些样本的病毒准种中占主导地位。表型分析显示,rtM204Q突变体具有89.9%的复制能力,其LAM EC₅₀比相应野生型毒株增加了76倍。相比之下,样本中的rtM204I突变体与rtM204Q突变体相比,复制能力较低,对LAM的耐药性更高(野生型毒株的复制能力为46.3%,LAM EC₅₀增加了1396倍)。rtM204Q突变体在体外对阿德福韦酯(ADV)敏感,在临床中对ADV/ADV + LAM挽救治疗敏感。

结论

rtM204Q被认为是一种新的与LAM耐药相关的突变。与rtM204I突变相比,它具有中等耐药性,且自然复制能力更强。

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