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慢性乙型肝炎和乙型肝炎相关肝硬化患者中新型 X 基因点突变。

Novel X gene point mutations in chronic hepatitis B and HBV related cirrhotic patients.

机构信息

Department of Microbiology, Torbat Jam Faculty of Medical Sciences, Torbat Jam, Iran.

Department of Microbiology, Golestan University of Medical Sciences, Gorgan, Iran.

出版信息

Infect Genet Evol. 2022 Jan;97:105186. doi: 10.1016/j.meegid.2021.105186. Epub 2021 Dec 14.

DOI:10.1016/j.meegid.2021.105186
PMID:34920100
Abstract

INTRODUCTION

HBx is a multifunctional modulator viral protein with key roles in various biological processes such as signal transduction, transcription, proliferation, and cell apoptosis. Also, HBx has an important role in the progression of cirrhosis and hepatocellular carcinoma (HCC). This study aimed to determine mutations in X gene, enhancer II (EnhII), and basal core promoter (BCP) of genotype D of Hepatitis B Virus (HBV) in cirrhotic and chronic HBV patients.

MATERIAL AND METHODS

This cross-sectional study was performed on 68 cases with chronic HBV (cHBV) and 50 cases with HBV related cirrhosis. Serum samples were obtained for genomic DNA extraction. Semi-nested PCR was used to amplify the HBx region. Point mutations in the HBx region were detected by sequencing.

RESULT

Novel mutations were detected, including C1491G, C1500T, G1613T, and G1658T in the N-terminal of the X gene. The frequency of C1481T/G1479A, T1498C, C1500T, G1512A, A1635T, C1678T, A1727T, and A1762T/ G1764A/ C1773T was significantly higher in cirrhotic patients compared to chronically HBV infected ones. A higher rate of A1635T, C1678T, A1727T, A1762T, G1764A, and C1773T was observed in cirrhotic patients.

CONCLUSION

Our findings showed that the frequency of mutations in the basal-core promoter, enhancer II, and regulatory region of the HBx gene was more seen in cirrhotic patients than in chronic HBV cases. Novel mutations were detected in the HBx gene, causing amino acid substitutions; however, the clinical impact of these novel mutations is yet to be cleared.

摘要

介绍

HBx 是一种多功能调节病毒蛋白,在信号转导、转录、增殖和细胞凋亡等多种生物学过程中具有关键作用。此外,HBx 在肝硬化和肝细胞癌(HCC)的进展中也具有重要作用。本研究旨在确定乙型肝炎病毒(HBV)基因型 D 的 X 基因、增强子 II(EnhII)和基本核心启动子(BCP)中的突变在肝硬化和慢性 HBV 患者中的情况。

材料和方法

这项横断面研究共纳入 68 例慢性 HBV(cHBV)患者和 50 例 HBV 相关肝硬化患者。采集血清样本提取基因组 DNA。采用半巢式 PCR 扩增 HBx 区。通过测序检测 HBx 区的点突变。

结果

在 X 基因的 N 端检测到新的突变,包括 C1491G、C1500T、G1613T 和 G1658T。与慢性 HBV 感染者相比,肝硬化患者中 C1481T/G1479A、T1498C、C1500T、G1512A、A1635T、C1678T、A1727T 和 A1762T/G1764A/C1773T 的频率明显更高。肝硬化患者中 A1635T、C1678T、A1727T、A1762T、G1764A 和 C1773T 的发生率更高。

结论

我们的研究结果表明,在肝硬化患者中,HBx 基因的基本核心启动子、增强子 II 和调节区的突变频率高于慢性 HBV 患者。在 HBx 基因中检测到新的突变,导致氨基酸取代;然而,这些新突变的临床影响尚不清楚。

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