Analysis of Hepatitis B virus (HBV) mutations in patients from Western Saudi Arabia with chronic disease

Analysis of Hepatitis B virus (HBV) mutations in patients from Western Saudi Arabia with chronic disease

Introduction: Extensive research has provided a link between HBV variants and the clinical complications of liver diseases. This study was performed to further investigate the relationship between HBV variants in preS, S and BCP/PC regions and disease progression in chronic hepatitis B (CHB) cases...

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Main Authors: Sherif Aly El-Kafrawy, Ghazi Abdulatif Jamjoom, Hisham Othman Akbar, Hind Ibrahim Baker Fallatah, Mai Mohamed El-Daly, Yousef Abdulfattah Qari, Abdullah Saeed Alghamdi, Mohamed Babatin, Mohammed Abdullah Alsaedi, Noura Abdulhamid Othman, Tagreed Lafi Al-Subhi, Mohamed Abdel-Hamid, Esam Ibraheem Azhar
Format: Article
Language:English
Published: The Journal of Infection in Developing Countries 2018-07-01
Series:Journal of Infection in Developing Countries
Subjects:
HBV
HBV variants
chronic HBV
sequencing
Saudi Arabia
Online Access:https://jidc.org/index.php/journal/article/view/9534
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Summary:Introduction: Extensive research has provided a link between HBV variants and the clinical complications of liver diseases. This study was performed to further investigate the relationship between HBV variants in preS, S and BCP/PC regions and disease progression in chronic hepatitis B (CHB) cases in Jeddah, Saudi Arabia. Methodology: 182 CHB patients were recruited for this study. HBV DNA was amplified by PCR in the PreS, S, and BCP/PC regions. Sequences were generated from 31 and 26 treated cases in PreS and S regions respectively and from 72 cases in the BCP/PC region. Results: The majority of cases (86.7%) were genotype D. Mutations at preS1-A2922C, X-A1624C and PC-G1887A were detected only in cases with either a high fibrosis score or hepatocellular carcinoma (HCC), while mutations at positions PC-C1982A, PC-G1951T, X-C1628T and X-A1630G were detected more frequently in HCC cases, without reaching statistical significance. Seven deletions were detected in the PreS-region. No deletions were detected in the CCAAT box. The accumulation of mutations per sample in the preS1-2 and S regions were associated with elevated ALT (p < 0.001, 0.001 and 0.001; respectively) and increased fibrosis (p = 0.018, 0.02 and 0.013; respectively). The accumulation of mutations per sample in the BCP/PC region is associated with high viral load. Occult hepatitis B infection (OBI) was identified in 5 samples. Conclusion: Our results add to the knowledge about HBV genotype-D variants. The accumulation of mutations per sample and OBI seem to play a role in the progression of HBV infection. G1896A was associated with the HBeAg negativity. The preS deletions did not play a role in liver disease progression.
ISSN:1972-2680

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