Scientific Reports (Feb 2021)

Sophisticated viral quasispecies with a genotype-related pattern of mutations in the hepatitis B X gene of HBeAg-ve chronically infected patients

  • Maria Francesca Cortese,
  • Carolina González,
  • Josep Gregori,
  • Rosario Casillas,
  • Luca Carioti,
  • Mercedes Guerrero-Murillo,
  • Mar Riveiro-Barciela,
  • Cristina Godoy,
  • Sara Sopena,
  • Marçal Yll,
  • Josep Quer,
  • Ariadna Rando,
  • Rosa Lopez-Martinez,
  • Beatriz Pacín Ruiz,
  • Selene García-García,
  • Rafael Esteban-Mur,
  • David Tabernero,
  • Maria Buti,
  • Francisco Rodríguez-Frías

DOI
https://doi.org/10.1038/s41598-021-83762-4
Journal volume & issue
Vol. 11, no. 1
pp. 1 – 11

Abstract

Read online

Abstract Patients with HBeAg-negative chronic infection (CI) have not been extensively studied because of low viremia. The HBx protein, encoded by HBX, has a key role in viral replication. Here, we analyzed the viral quasispecies at the 5′ end of HBX in CI patients and compared it with that of patients in other clinical stages. Fifty-eight HBeAg-negative patients were included: 16 CI, 19 chronic hepatitis B, 16 hepatocellular carcinoma and 6 liver cirrhosis. Quasispecies complexity and conservation were determined in the region between nucleotides 1255 and 1611. Amino acid changes detected were tested in vitro. CI patients showed higher complexity in terms of mutation frequency and nucleotide diversity and higher quasispecies conservation (p < 0.05). A genotype D-specific pattern of mutations (A12S/P33S/P46S/T36D-G) was identified in CI (median frequency, 81.7%), which determined a reduction in HBV DNA release of up to 1.5 log in vitro. CI patients showed a more complex and conserved viral quasispecies than the other groups. The genotype-specific pattern of mutations could partially explain the low viremia observed in these patients.