尼日利亚伊巴丹 HBsAg 阳性患者中 HBV 基因型的多样性及其与前核心/基本核心突变的关系。

Access microbiology Pub Date : 2024-11-07 eCollection Date: 2024-01-01 DOI:10.1099/acmi.0.000821.v3
Adedayo Omotayo Faneye, Babatunde Olanrewaju Motayo, Aisha Mustafa, Georgina Odiabo
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摘要

背景。乙型肝炎病毒(HBV)是导致全球严重肝病和肝细胞癌的最主要原因。研究表明,乙型肝炎病毒的基础核心蛋白(BCP)和前核心蛋白(PC)在乙型肝炎病毒相关致癌过程中发挥着重要作用。有关尼日利亚 BCP 和 PC 突变的类型和影响的数据很少。本研究旨在对尼日利亚伊巴丹的 HBV 患者进行基因分型,并调查 BCP 和 PC 是否存在突变。研究方法本研究招募了 40 名 HBV DNA 阳性患者,通过巢式多重 PCR 进行病毒载量检测和基因分型。对部分 X 基因区进行了扩增和 Sanger 测序。然后利用生物信息学对 BPC 和 PC 基因组区域进行分析。结果23 名参与者的 HBV DNA 病毒载量大于 20 000 IU,17 名有结论。我们报告了一个多样化的 HBV 遗传景观,BCP 双突变 A1762T/G1764A 基因型之间存在混合感染,这预示着 HBV 相关肝病预后不良的可能性。我们的研究结果有助于我们了解 HBV 的分子特征及其对尼日利亚 HBV 感染者疾病进展和管理的潜在影响。
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Diversity of HBV genotypes and their association with precore/basal core mutations among HBsAg-positive patients in Ibadan, Nigeria.

Background. Hepatitis B virus (HBV) is the most implicated cause of severe liver disease and hepatocellular carcinoma worldwide. Studies have shown that the basal core protein (BCP) and precore protein (PC) of HBV play a significant role in HBV-related carcinogenesis. There is a paucity of data on the type and effect of BCP and PC mutations in Nigeria. This study aims to genotype HBV and investigate any mutations within the BCP and PC among HBV patients in Ibadan, Nigeria. Methods. Forty HBV-DNA-positive patients were recruited into this study, and the viral load assay and genotyping by nested multiplex PCR were done. The partial X gene region was amplified and Sanger sequenced. The BPC and PC genomic regions were then analysed using bioinformatics. Results. Twenty-three participants recorded HBV DNA viral load of >20 000 IU, while 17 had <20 000 IU and 28 samples were genotyped. Five genotypes (A, B, C, D and E) and four mixed genotypes (AC, AD ACD and ABCD) were detected. Genotype AC was the most frequently encountered, while genotypes E and B were the least encountered. Mutation was highest in ages 34-45 years. Double mutation A1762T and G1764A within the BCP region was the most encountered mutation. Conclusions. We report a diverse HBV genetic landscape, with mixed infections between genotypes with BCP double-mutation A1762T/G1764A, signalling the likelihood of poor HBV-related liver disease prognosis. Our findings contribute to our understanding of the molecular characteristics of HBV and its potential implications for disease progression and management among HBV-infected Nigerians.

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