Hepatitis B virus escape mutants: “pushing the envelope” of chronic hepatitis B virus infection

Hepatitis B virus (HBV) DNA was extracted from sera of six carriers with hepatitis B e antigen as well as antibody to hepatitis B surface antigen and sequenced within the pre‐S regions and the S gene. HBV DNA clones from five of these carriers had point mutations in the S gene, resulting in conversion from IIe‐126 or Thr‐126 of the wild‐type virus to Ser‐126 or Asn‐126 in three carriers and conversion from Gly‐145 to Arg‐145 in three of them; clones with Asn‐126 or Arg‐145 were found in one carrier. All 12 clones from the other carrier had an insertion of 24 bp encoding an additional eight amino acids between Thr‐123 and Cys‐124. In addition, all or at least some of the HBV DNA clones from these carriers had inphase deletions in the 5′ terminus of the pre‐S2 region. These results indicate that HBV escape mutants with mutations in the S gene affecting the expression of group‐specific determinants would survive in some carriers after they seroconvert to antibody against surface antigen. Carriers with HBV escape mutants may transmit HBV either by donation of blood units without detectable surface antigen or through community‐acquired infection, which would hardly be prevented by current hepatitis B immunoglobulin or vaccines.