谷丙转氨酶（ALT）水平持续升高或正常的D基因型乙型肝炎病毒患者核心启动子和前核心区域的核苷酸差异

Nucleotide divergences in the core promoter and precore region of genotype D hepatitis B virus in patients with persistently elevated or normal ALT levels.

作者信息

Bozdayi A M, Bozkaya H, Türkyilmaz A R, Sarýodlu M, Cetinkaya H, Karayalçin S, Yurdaydin C, Uzunalimoğlu O

机构信息

Ankara University, Institute of Hepatology, School of Medicine, Department of Gastroenterology, 06100 Cebeci, Ankara, Turkey.

出版信息

J Clin Virol. 2001 Apr;21(1):91-101. doi: 10.1016/s1386-6532(01)00148-2.

DOI:10.1016/s1386-6532(01)00148-2

PMID:11255102

Abstract

BACKGROUND

Mutation in the hepatitis B virus precore codon 28, creating a translational stop codon and double 1762-1764 T/A mutations in the core promoter region, controlling the transcription of the precore RNA and the core RNA have been suggested to correlate with the HBeAg status of patients with HBV infection.

OBJECTIVES

The aim of the study was to further investigate the association of nucleotide divergences in both core promoter and precore regions with liver cell injury (reflected by ALT levels) in patients with chronic HBV infection.

STUDY DESIGN

The sequences of the core promoter and the precore region of HBV isolated from 67 patients, all having genotype D and subtype ayw were analyzed. The patients were divided into two groups and four subgroups according to their HBeAg and Anti-HBe status, and ALT profile.

RESULTS

It was found that the nucleotide divergences in the core promoter but not in the precore region were higher in patients having persistently elevated serum ALT than in serum ALT normal patients in both HBeAg positive and Anti-HBe positive groups (P<0.05). The number of T/A and A1896 stop codon mutations did not yield a statistically significant difference between ALT normal and elevated groups. It was also found that 1762-1764 T/A and precore A 1896 mutation existed in five and six out of 29 HBeAg positive patients, respectively. In 38 anti-HBe positive patients, 1762-1764 T/A and precore A1896 mutation were detected in three and 16 patients respectively, and coexisted in 10 patients.

CONCLUSIONS

Precore A 1896 stop codon mutation seems to play an essential role in the loss of HBeAg in Turkish patients. Serum viremia levels of HBV in patients having precore stop codon and/or T/A mutation were not significantly different from the other patients carrying wild type strains. Nucleotide variability in the core promoter region may be one of the factors linked to hepatitis B disease activity.

摘要

背景

乙型肝炎病毒前核心密码子28处的突变会产生一个翻译终止密码子，并且核心启动子区域存在1762 - 1764位的T/A双突变，这些突变控制前核心RNA和核心RNA的转录，已被认为与乙肝病毒感染患者的HBeAg状态相关。

目的

本研究的目的是进一步探究慢性乙肝病毒感染患者核心启动子和前核心区域的核苷酸差异与肝细胞损伤（以ALT水平反映）之间的关联。

研究设计

分析了从67例均为D基因型和ayw亚型的患者中分离出的乙肝病毒核心启动子和前核心区域的序列。根据患者的HBeAg和抗 - HBe状态以及ALT情况，将患者分为两组和四个亚组。

结果

发现在HBeAg阳性和抗 - HBe阳性组中，血清ALT持续升高的患者核心启动子区域的核苷酸差异高于血清ALT正常的患者，而前核心区域则无此差异（P<0.05）。T/A和A1896终止密码子突变的数量在ALT正常组和升高组之间没有统计学上的显著差异。还发现，29例HBeAg阳性患者中有5例存在1762 - 1764 T/A突变，6例存在前核心A1896突变。在38例抗 - HBe阳性患者中，分别有3例和16例检测到1762 - 1764 T/A突变和前核心A1896突变，10例患者两者共存。