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乙肝e抗原血清学转换期间的病毒准种进化

Viral quasi-species evolution during hepatitis Be antigen seroconversion.

作者信息

Lim Seng Gee, Cheng Yan, Guindon Stephane, Seet Bee Leng, Lee Lay Yong, Hu Peizhen, Wasser Shanthi, Peter Frank Josef, Tan Theresa, Goode Matthew, Rodrigo Allen Gerard

机构信息

Department of Gastroenterology and Hepatology, National University Hospital, Singapore.

出版信息

Gastroenterology. 2007 Sep;133(3):951-8. doi: 10.1053/j.gastro.2007.06.011. Epub 2007 Jun 20.

Abstract

BACKGROUND & AIMS: Although viral quasi-species evolution may be related to pathogenesis of disease, little is known about this in hepatitis B virus (HBV); consequently, we aimed to evaluate the evolution of HBV quasi-species in patients with well-characterized clinical phenotypes of chronic hepatitis B.

METHODS

Four cohorts of well-defined clinical phenotypes of chronic hepatitis B, hepatitis Be antigen (HBeAg) seroconverters (spontaneous seroconverters and interferon-induced seroconverters) and nonseroconverters (controls and interferon nonresponders) were followed during 60 months on average. Serum from 4 to 5 time points was used for nested polymerase chain reaction, cloning, and sequencing of the precore/core gene (20 clones/sample). Only patients with genotype B were used. Sequences were aligned using Clustal X, then serial-sample unweighted pair grouping method with arithmetic means phylogenetic trees were constructed using Pebble 1.0 after which maximum likelihood estimates of pairwise distances under a GTR + I + G model was assessed. Viral diversity and substitution rates were then estimated.

RESULTS

Analysis of 3386 sequences showed that HBeAg seroconverters had 2.4-fold higher preseroconversion viral sequence diversity (P = .0183), and 10-fold higher substitution rate (P < .0001) than did nonseroconverters, who had persistently low viral diversity (3.6 x 10(-3) substitutions/site) and substitution rate (2.2 x 10(-5) substitutions x site(-1) x month(-1)). After seroconversion, there was a striking increase in viral diversity. Most seroconverters had viral variants that showed evidence of positive selection, which was seen mainly after seroconversion.

CONCLUSIONS

The high viral diversity before a reduction in HBV DNA and before HBeAg seroconversion could either be related to occurrence of stochastic mutations that lead to a break in immune tolerance or to increased immune reactivity that drives escape mutations.

摘要

背景与目的

尽管病毒准种进化可能与疾病发病机制有关,但对于乙型肝炎病毒(HBV)的这方面情况知之甚少;因此,我们旨在评估慢性乙型肝炎临床表型明确的患者中HBV准种的进化情况。

方法

对四组慢性乙型肝炎临床表型明确的患者进行平均60个月的随访,这些患者包括HBeAg血清学转换者(自发血清学转换者和干扰素诱导血清学转换者)以及非血清学转换者(对照组和干扰素无应答者)。采集4至5个时间点的血清,用于前核心/核心基因的巢式聚合酶链反应、克隆及测序(每个样本20个克隆)。仅纳入B基因型患者。使用Clustal X对序列进行比对,然后用Pebble 1.0构建算术平均法的序列样本非加权配对分组法系统发育树,之后在GTR + I + G模型下评估成对距离的最大似然估计值。然后估计病毒多样性和替代率。

结果

对3386个序列的分析表明,HBeAg血清学转换者在血清学转换前的病毒序列多样性比非血清学转换者高2.4倍(P = 0.0183),替代率高10倍(P < 0.0001),非血清学转换者的病毒多样性持续较低(3.6×10⁻³ 替代/位点),替代率也较低(2.2×10⁻⁵ 替代×位点⁻¹×月⁻¹)。血清学转换后,病毒多样性显著增加。大多数血清学转换者具有显示正选择证据的病毒变体,这主要在血清学转换后出现。

结论

在HBV DNA降低和HBeAg血清学转换之前的高病毒多样性,可能与导致免疫耐受打破的随机突变发生有关,或者与驱动逃逸突变的免疫反应性增加有关。

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