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 (<12. IU/ml). 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 < 12 IU/ml. 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.
Lamivudine-resistance mutations can be selected even at very low levels of hepatitis B viraemia / V. Svicher, C. Alteri, C. Gori, R. Salpini, F. Marcuccilli, A. Bertoli, R. Longo, M. Bernassola, V. Gallinaro, S. Romano, M. Visca, A. Ursitti, M. Feasi, V. Micheli, M. Angelico, G. Cassola, G. Parruti, G. Gubertini, G.M. De Sanctis, F. Ceccherini-Silberstein, G. Cappiello, A. Spano, C.F. Perno. - In: DIGESTIVE AND LIVER DISEASE. - ISSN 1590-8658. - 42:12(2010), pp. 902-907.
Lamivudine-resistance mutations can be selected even at very low levels of hepatitis B viraemia
C. Alteri;C.F. Perno
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 (<12. IU/ml). 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 < 12 IU/ml. 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.
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