| Literature DB >> 15339340 |
Eneida A Santos1, Michel V F Sucupira, Juçara Arabe, Selma A Gomes.
Abstract
BACKGROUND: Lamivudine inhibits replication of both human immunodeficiency virus (HIV) and hepatitis B virus (HBV) and is commonly used as part of antiretroviral therapy. The main limitation in the use of lamivudine is resistant mutation selection. Most of these mutations affect the YMDD motif of the HBV DNA polymerase. The resistance occurs through M550V or M550I aminoacid replacements. The M550V variation may be accompanied by L526M mutation, notably in HIV-HBV co-infected patients. The aim of this study was to investigate mutations associated with lamivudine resistance in a hemodialysis patient chronically co-infected with HIV-1 and HBV, who was submitted to several antiretroviral treatments.Entities:
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Year: 2004 PMID: 15339340 PMCID: PMC516776 DOI: 10.1186/1471-2334-4-29
Source DB: PubMed Journal: BMC Infect Dis ISSN: 1471-2334 Impact factor: 3.090
Figure 1HBV load (vertical bars) and ALT levels (curve) during antiretroviral therapies.
Figure 2Phylogenetic tree of HBV isolates constructed with the neighbor-joining method, and based on the nucleotide sequences of the entire pre-S/S region (nt positions 2854 to 833). Isolates whose names begin by 1,2,3 were molecular clones from this study derived from samples collected in 1999, 2001, and 2002, respectively. The other isolates are designated by their GenBank accession numbers. Genotype A isolates clustered in two subgroups, designated A-A' (genotype A excluding A') and A' [27]. The sequence AY090458 belongs to genotype F and was used as an outgroup. Numbers at internal nodes indicate percentage of 100 bootstrap replicates that support the branch. Only values > 85% are indicated. The horizontal bar provides a genetic distance.
Amino acid replacements in polymerase and surface antigen (small S)
| Year of collect | Lamivudine | HBV sequences | Polymerase residues | S residues | |||||||||
| 359 | 473 | 519 | 526 | 550 | 100 | 119 | 164 | 182 | 195 | 216 | |||
| 1999 | Yes | Direct | Y | G | V | C | G | E | W | L | |||
| 1-B40 | Y | G | V | C | G | E | W | L | |||||
| 1-B52 | Y | G | V | C | G | E | W | L | |||||
| 1-B57 | Y | G | C | G | W | L | |||||||
| 2001 | No | Direct | Y | E | V | L | M | C | R | E | W | I | L |
| 2-B14 | Y | E | V | L | M | C | R | E | * | I | L | ||
| 2-B62 | Y | E | V | L | M | C | R | E | W | I | * | ||
| 2-B63 | Y | E | V | L | M | C | R | E | W | I | L | ||
| 2002 | Yes | Direct | Y | G | C | G | W | L | |||||
| 3-B02 | Y | G | C | G | W | L | |||||||
| 3-B06 | Y | G | C | G | W | L | |||||||
| 3-B71 | Y | G | C | G | W | L | |||||||
| H | G | V | L | M | Y | G | E | W | I | L | |||
Lamivudine resistant mutations in the viral DNA polymerase and their counterparts in the small surface antigen are marked in bold. Asterisks represent stop mutations.