4.6 Article

Characterization of Antigen Escape Mutations in Chronic HBV-Infected Patients in Upper Egypt

Journal

INFECTION AND DRUG RESISTANCE
Volume 14, Issue -, Pages -

Publisher

DOVE MEDICAL PRESS LTD
DOI: 10.2147/IDR.S315299

Keywords

HBV; a determinant; mutational analysis; vaccine escape; Upper Egypt

Funding

  1. Science, Technology & Innovation Funding Authority (STDF) [30208]

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In Upper Egypt, genotype D was found to be the major circulating type among chronic HBV-infected patients, with mutations in the a determinant region only detected in genotype D isolates. This could pose a potential threat to HBV diagnosis, therapy success, and vaccination programs in Upper Egypt.
Background: Mutations within the a determinant region (position 124-147) that is present in the major hydrophilic region (MHR, position 99-160) of the hepatitis B surface antigen (HBsAg) are associated with vaccine-escape, lack of diagnosis, and failure to hepatitis B immunoglobulin (HBIG) therapy. Data regarding the amino acid changes of a determinant region of HBsAg are limited in Egypt. The prevalence and mutations in this region among chronic HBV (CHB)infected patients in Upper Egypt are not known. Material and Methods: Blood samples were collected from HBsAg-positive CHB-infected patients (n=123) admitted to Assiut University Hospitals. Serum samples were screened for HBsAg, HBeAg, anti-HBs and anti-HBe antibodies using commercially available ELISA kits. Viral load was determined by qPCR. In addition, mutational analysis was carried out targeting the HBV surface gene to determine the HBV genotype and vaccine escape mutations. Results: Sequencing analysis of HBV DNA revealed that genotype D is the major circulating type (81.3%), followed by genotype E (18.7%). Analysis of the HBV genome revealed that 103/123 (83.7%) patients showed wild-type sequences and 20/123 (16.3%) showed mutations in the HBsAg gene. Mutation in seventeen patients (17/20, 85%) showed only one mutation, and three patients showed two mutations (3/20, 15%) in the a determinant region. The observed mutations were T115S (3/20, 15%), P120T/S (3/20, 15%), T126S (1/ 20, 5%), Q129R (2/20, 10%), M133T (2/20, 10%), S143L (5/20, 25%), D144E/A (3/20, 15%), and G145R/A (4/20, 20%). Mutations in the a determinant region were detected in genotype D isolates only. Conclusion: We described for the first time the prevalence and characterization of vaccine escape mutants in CHB patients in Upper Egypt. Mutational analysis of the a determinant region revealed the presence of a wide spectrum of mutants in the circulating HBV isolates that could be a potential threat to HBV diagnosis, therapy success, and HBV vaccination program in Upper Egypt.

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