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快速检测乙型肝炎病毒基因组前核心启动子和前核心区域的基因型及突变:与病毒持续性及疾病严重程度的相关性

Rapid detection of genotypes and mutations in the pre-core promoter and the pre-core region of hepatitis B virus genome: correlation with viral persistence and disease severity.

作者信息

Grandjacques C, Pradat P, Stuyver L, Chevallier M, Chevallier P, Pichoud C, Maisonnas M, Trépo C, Zoulim F

机构信息

Liver Unit, Hôtel-Dieu, Lyon, France.

出版信息

J Hepatol. 2000 Sep;33(3):430-9. doi: 10.1016/s0168-8278(00)80279-2.

Abstract

BACKGROUND/AIMS: We aimed to clarify the clinical relevance of hepatitis B virus pre-core mutant detection in patients with chronic hepatitis B using a newly developed assay.

METHODS

Viral genotypes and pre-core mutations were studied in relation to viral persistence and liver disease severity using INNO-LiPA methodology. The study group included 151 patients with chronic hepatitis B, 85 positive for HBeAg (group I) and 66 positive for anti-HBe (group II).

RESULTS

The prevalence of viral genotypes in group I was: 64% A, 1% B, 15% C, 19% D, 0% E, 0% F and in group II: 39% A, 0% B, 2% C, 56% D, 2% E, 2% F (p<0.001). The prevalence of mutations at pre-core codon 28 (M2) was lower in group I (5%) than in group II (64%) (p<0.001). The prevalence of pre-core promoter mutations was also lower in group I (21%) than in group II (61%) (p<0.001). M2 mutations were more frequently detected in genotype D than in genotype A (p<0.001), while the other mutations were not influenced by viral genotype. Serum HBV DNA levels were significantly lower in group II versus group I (p<0.001), and in patients with any of the pre-core mutations versus wild-type sequence (p<0.01). Although cirrhosis was more frequent in group II (37%) versus group I (22%) and in patients with either one of the pre-core mutation (31%) versus wild-type sequence (25%), there was no statistical difference in liver severity assessed by ALT levels and Knodell score.

CONCLUSION

Pre-core mutants, whose molecular pattern is strongly dependent on viral genotypes, are associated with viral persistence in anti-HBe positive patients with ongoing chronic hepatitis B. The availability of this rapid assay should allow a precise monitoring of viral pre-core mutants during the course of chronic hepatitis B.

摘要

背景/目的:我们旨在通过一种新开发的检测方法,阐明慢性乙型肝炎患者中乙肝病毒前核心区突变检测的临床相关性。

方法

使用INNO-LiPA方法研究病毒基因型和前核心区突变与病毒持续存在及肝病严重程度的关系。研究组包括151例慢性乙型肝炎患者,85例HBeAg阳性(I组),66例抗-HBe阳性(II组)。

结果

I组病毒基因型的流行率为:64%A、1%B、15%C、19%D、0%E、0%F;II组为:39%A、0%B、2%C、56%D、2%E、2%F(p<0.001)。I组前核心区密码子28(M2)突变的流行率(5%)低于II组(64%)(p<0.001)。I组前核心区启动子突变的流行率(21%)也低于II组(61%)(p<0.001)。M2突变在D基因型中比在A基因型中更频繁地被检测到(p<0.001),而其他突变不受病毒基因型影响。II组血清HBV DNA水平显著低于I组(p<0.001),并且在任何前核心区突变患者中低于野生型序列患者(p<0.01)。虽然II组(37%)肝硬化比I组(22%)更常见,并且在前核心区突变之一的患者中(31%)比野生型序列患者(25%)更常见,但通过ALT水平和Knodell评分评估的肝脏严重程度没有统计学差异。

结论

前核心区突变体,其分子模式强烈依赖于病毒基因型,与抗-HBe阳性的慢性乙型肝炎患者的病毒持续存在相关。这种快速检测方法的可用性应能在慢性乙型肝炎病程中精确监测病毒前核心区突变体。

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