Impaired HBsAg release and antiproliferative/antioxidant cell regulation by HBeAg-negative patient isolates reflects an evolutionary process.
Michael BasicKeerthihan ThiyagarajahMirco GlitscherAnja SchollmeierQingyan WuEsra GörgülüPia LembeckJannik SonnenbergJulia DietzFabian FinkelmeierMichael PraktiknjoJonel TrebickaStefan ZeuzemChristoph SarrazinEberhard HildtKai-Henrik PeifferPublished in: Liver international : official journal of the International Association for the Study of the Liver (2024)
HBeAg-negative genomes from Phase 3 exhibit distinct molecular characteristics leading to lower HBsAg synthesis and release, enhanced oxidative stress protection and decreased activity of key kinases, triggering an antiproliferative stage, which might contribute to the lower probability of hepatocellular carcinoma. The observed differences cannot be associated with loss of HBeAg or specific mutations common to all analysed isolates, indicating the phenotype of Phase 3 derived genomes to be the result of a multifactorial process likely reflecting a conserved natural selection process.