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Lamivudine-resistance mutations can be selected even at very low levels of hepatitis B viraemia

Authors :
Valentina Svicher
Giuseppe Maria De Sanctis
Francesca Ceccherini-Silberstein
Carlo Federico Perno
Antonella Ursitti
Marcello Feasi
Giovanni Cassola
R. Longo
Valentina Gallinaro
Ada Bertoli
Claudia Alteri
Mario Angelico
Fabbio Marcuccilli
Alberto Spanò
Giustino Parruti
Caterina Gori
M. Visca
Romina Salpini
Giuseppina Cappiello
Valeria Micheli
S. Romano
M. Bernassola
Guido Gubertini
Publication Year :
2010
Publisher :
Elsevier Science Limited, 2010.

Abstract

Objective To investigate lamivudine (LAM)-resistance profiles of hepatitis B virus (HBV) at the early stages of virological breakthrough (serum HBV-DNA 12–345 IU/ml) or when HBV-DNA is undetectable. Methods Sixty-four HBV-mono-infected patients were enrolled: 25 had virological breakthrough with serum HBV-DNA ranging from 12 to 345 IU/ml during first-line LAM-monotherapy; 24 were on LAM-monotherapy, and 15 were on LAM + adefovir dipivoxil (ADV) with undetectable serum HBV-DNA ( Results HBV-reverse transcriptase was successfully sequenced in 22 (88.0%) LAM-treated patients with HBV-DNA between 12 and 345 IU/ml, and in 12 (30.8%) patients receiving LAM (±ADV) with HBV-DNA Drug-resistance mutations were observed in 17 (77.2%) LAM-treated patients with virological breakthrough: 8 M204V, 7 M204I, 1 M204I/V, and 1 A181T. One or ≥2 compensatory mutations were found in 10 (58.8%) and in 4 (23.5%) patients. Drug-resistance mutations were present also in patients with undetectable serum HBV-DNA: M204I was detected in 2 patients receiving LAM-monotherapy, and V84M in 1 patient receiving LAM + ADV. Conclusion Overall findings support the existence of drug-resistance mutations even at very low levels of viral replication. The persistence of low-level HBV replication and consequent drug-resistance emergence should be considered when choosing therapeutic strategies.

Details

Language :
English
Database :
OpenAIRE
Accession number :
edsair.doi.dedup.....6f2c8cbc4383ea4a92bc3137de0ec35a