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乙型肝炎病毒核心蛋白 S21 取代与暴发性肝炎的关系。

Association between S21 substitution in the core protein of hepatitis B virus and fulminant hepatitis.

机构信息

Division of Gastroenterology, Tohoku University Graduate School of Medicine, Sendai, Japan.

出版信息

J Clin Virol. 2012 Oct;55(2):147-52. doi: 10.1016/j.jcv.2012.06.011. Epub 2012 Jul 12.

Abstract

BACKGROUND

The viral factors of hepatitis B virus (HBV), such as genotypes and mutations, were reported to affect the development of fulminant hepatitis B (FHB), but the mechanism is still unclear.

OBJECTIVES

To investigate HBV mutations associated with FHB, especially in the subgenotype B1/Bj HBV (HBV/B1), which are known to cause FHB frequently in Japan.

STUDY DESIGN

A total of 96 serum samples from acute self-limited hepatitis B (AHB) patients and 13 samples from FHB patients were used for full-genome/partial sequencing. A total of 107 chronic infection patients with HBV were also examined for the distribution of mutants.

RESULTS

In the analysis of full-genome sequences of HBV/B1 (FHB, n=11; non-FHB, n=35) including those from the databases, mutations at nt 1961 [T1961V (not T)] and nt 1962 [C1962D (not C)], which change S21 in the core protein, were found more frequently in FHB than in non-FHB (100% vs. 20%, 55% vs. 3%, respectively). When our FHB and AHB samples were compared, T1961V and C1962D were significantly more frequent in FHB than in AHB, both in the overall analysis (46% vs. 6%, 39% vs. 3%, respectively) and in HBV/B1 (100% vs. 29%, 100% vs. 14%, respectively). A newly developed PCR system detecting T1961V showed that HBV/B1 and low viral load were independent factors for the mutation among chronic infection patients.

CONCLUSIONS

T1961V/C1962D mutations were found frequently in FHB, especially in HBV/B1. The resulting S21 substitution in the core protein may play important roles in the development of FHB.

摘要

背景

乙型肝炎病毒(HBV)的病毒因素,如基因型和突变,据报道会影响暴发性乙型肝炎(FHB)的发展,但机制尚不清楚。

目的

研究与 FHB 相关的 HBV 突变,特别是在亚基因型 B1/Bj HBV(HBV/B1)中,已知其在日本常引起 FHB。

研究设计

共使用 96 份来自急性自限性乙型肝炎(AHB)患者和 13 份来自 FHB 患者的血清样本进行全基因组/部分测序。还检查了 107 例慢性 HBV 感染患者突变的分布情况。

结果

在对 HBV/B1(FHB,n=11;非 FHB,n=35)的全基因组序列(包括数据库中的序列)分析中,发现核心蛋白中 S21 发生改变的 nt1961[T1961V(非 T)]和 nt1962[C1962D(非 C)]突变在 FHB 中比在非 FHB 中更为常见(100%比 20%,55%比 3%)。当比较我们的 FHB 和 AHB 样本时,T1961V 和 C1962D 在 FHB 中比在 AHB 中更为常见,无论是在总体分析中(46%比 6%,39%比 3%)还是在 HBV/B1 中(100%比 29%,100%比 14%)。一种新开发的检测 T1961V 的 PCR 系统显示,HBV/B1 和低病毒载量是慢性感染患者发生突变的独立因素。

结论

在 FHB 中发现了 T1961V/C1962D 突变,特别是在 HBV/B1 中。核心蛋白中 S21 取代可能在 FHB 的发展中发挥重要作用。

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