TY - JOUR
T1 - Protease mutation M89I/V is linked to therapy failure in patients infected with the HIV-1 non-B subtypes C, F or G
AU - Abecasis, Ana Barroso
AU - Deforche, Koen
AU - Snoeck, Joke
AU - Bacheler, Lee T.
AU - McKenna, Paula
AU - Carvalho, Ana Patrícia
AU - Gomes, Perpétua
AU - Camacho, Ricardo Jorge
AU - Vandamme, Anne Mieke
PY - 2005/11/4
Y1 - 2005/11/4
N2 - Objective: To investigate whether and how mutations at position 89 of HIV-1 protease were associated with protease inhibitor (PI) failure, and what is the impact of the HIV-1 subtype. Methods: In a database containing pol nucleotide sequences and treatment history, the correlation between PI experience and mutations at codon 89 was determined separately for subtype B and several non-B subtypes. A Bayesian network model was used to map the resistance pathways in which M89I/V is involved for subtype C. The phenotypic effect of M89I/V for several PIs was also measured. Results: The analysis showed that for the subtypes C, F and G in which the wild-type codon at 89 was M compared to L for subtype B, M89I/V was significantly more frequently observed in PI-treated patients displaying major resistance mutations to PIs than in drug-naive patients. M89I/V was strongly associated with PI resistance mutations at codons 71, 74 and 90. Phenotypically, M89I/V alone did not confer a reduced susceptibility to PIs. However, when combined with L90M, a significantly reduced susceptibility to nelfinavir was observed (P < 0.05) in comparison with strains with L90M alone. Conclusions: The results of the present study show that M89I/V is associated with PI experience in subtypes C, F and G but not in subtype B. M89I/V should be considered a secondary PI mutation with an important effect on nelfinavir susceptibility in the presence of L90M.
AB - Objective: To investigate whether and how mutations at position 89 of HIV-1 protease were associated with protease inhibitor (PI) failure, and what is the impact of the HIV-1 subtype. Methods: In a database containing pol nucleotide sequences and treatment history, the correlation between PI experience and mutations at codon 89 was determined separately for subtype B and several non-B subtypes. A Bayesian network model was used to map the resistance pathways in which M89I/V is involved for subtype C. The phenotypic effect of M89I/V for several PIs was also measured. Results: The analysis showed that for the subtypes C, F and G in which the wild-type codon at 89 was M compared to L for subtype B, M89I/V was significantly more frequently observed in PI-treated patients displaying major resistance mutations to PIs than in drug-naive patients. M89I/V was strongly associated with PI resistance mutations at codons 71, 74 and 90. Phenotypically, M89I/V alone did not confer a reduced susceptibility to PIs. However, when combined with L90M, a significantly reduced susceptibility to nelfinavir was observed (P < 0.05) in comparison with strains with L90M alone. Conclusions: The results of the present study show that M89I/V is associated with PI experience in subtypes C, F and G but not in subtype B. M89I/V should be considered a secondary PI mutation with an important effect on nelfinavir susceptibility in the presence of L90M.
KW - M89I/V
KW - Mutation
KW - Non-B subtypes
KW - Protease
KW - Resistance
UR - http://www.scopus.com/inward/record.url?scp=27544477733&partnerID=8YFLogxK
U2 - 10.1097/01.aids.0000188422.95162.b7
DO - 10.1097/01.aids.0000188422.95162.b7
M3 - Article
C2 - 16227787
AN - SCOPUS:27544477733
SN - 0269-9370
VL - 19
SP - 1799
EP - 1806
JO - AIDS
JF - AIDS
IS - 16
ER -