Emerging Microbes and Infections (Dec 2023)

Unexpected rise in the circulation of complex HBV variants enriched of HBsAg vaccine-escape mutations in HBV genotype-D: potential impact on HBsAg detection/quantification and vaccination strategies

  • Lorenzo Piermatteo,
  • Stefano D’Anna,
  • Ada Bertoli,
  • Maria Bellocchi,
  • Luca Carioti,
  • Lavinia Fabeni,
  • Mohammad Alkhatib,
  • Simone La Frazia,
  • Miriam Lichtner,
  • Claudio Mastroianni,
  • Giuseppe De Sanctis,
  • Massimo Marignani,
  • Caterina Pasquazzi,
  • Nerio Iapadre,
  • Giustino Parruti,
  • Giuseppina Cappiello,
  • Jacopo Vecchiet,
  • Vincenzo Malagnino,
  • Sandro Grelli,
  • Francesca Ceccherini-Silbertein,
  • Massimo Andreoni,
  • Loredana Sarmati,
  • Valentina Svicher,
  • Romina Salpini

DOI
https://doi.org/10.1080/22221751.2023.2219347
Journal volume & issue
Vol. 12, no. 1

Abstract

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ABSTRACTSpecific HBsAg mutations are known to hamper HBsAg recognition by neutralizing antibodies thus challenging HBV-vaccination efficacy. Nevertheless, information on their impact and spreading over time is limited. Here, we characterize the circulation of vaccine-escape mutations from 2005 to 2019 and their correlation with virological parameters in a large cohort of patients infected with HBV genotype-D (N = 947), dominant in Europe. Overall, 17.7% of patients harbours ≥1 vaccine-escape mutation with the highest prevalence in subgenotype-D3. Notably, complex profiles (characterized by ≥2 vaccine-escape mutations) are revealed in 3.1% of patients with a prevalence rising from 0.4% in 2005–2009 to 3.0% in 2010–2014 and 5.1% in 2015–2019 (P = 0.007) (OR[95%CI]:11.04[1.42–85.58], P = 0.02, by multivariable-analysis). The presence of complex profiles correlates with lower HBsAg-levels (median[IQR]:40[0–2905]IU/mL for complex profiles vs 2078[115–6037]IU/ml and 1881[410–7622]IU/mL for single or no vaccine-escape mutation [P < 0.02]). Even more, the presence of complex profiles correlates with HBsAg-negativity despite HBV-DNA positivity (HBsAg-negativity in 34.8% with ≥2 vaccine-escape mutations vs 6.7% and 2.3% with a single or no vaccine-escape mutation, P < 0.007). These in-vivo findings are in keeping with our in-vitro results showing the ability of these mutations in hampering HBsAg secretion or HBsAg recognition by diagnostic antibodies. In conclusion, vaccine-escape mutations, single or in complex profiles, circulate in a not negligible fraction of HBV genotype-D infected patients with an increasing temporal trend, suggesting a progressive enrichment in the circulation of variants able to evade humoral responses. This should be considered for a proper clinical interpretation of HBsAg-results and for the development of novel vaccine formulations for prophylactic and therapeutic purposes.

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