Interpretation of Genotype and Pharmacokinetics for Resistance to Fosamprenavir-Ritonavir-Based Regimens in Antiretroviral-Experienced Patients

Pellegrin, Isabelle; Breilh, Dominique; Coureau, Gaëlle; Boucher, Sébastien; Néau, Didier; Merel, Patrick; Lacoste, D.; Fleury, Hervé; Saux, Marie-Claude; Pellegrin, Jean‐Luc; Lazaro, Estibaliz; Dabis, François; Thiébaut, Rodolphe

doi:10.1128/aac.00481-06

Cited by 22 publications

(19 citation statements)

References 34 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…The M36I mutation is the only polymorphic mutation in the C-SA protease that is associated with drug resistance to most of the FDAapproved PIs in combination with ritonavir [41]. This mutation is associated with virological failure or a reduced virological response to atazanavir, darunavir, fosamprenavir, indinavir, lopinavir, saquinavir and tipranavir in combination with ritonavir [42][43][44][45][46][47][48][49]. Mutations at residue position 89 are associated with virological failure to darunavir and tipranavir in combination with ritonavir [44,50], and mutations at resi- In the subtype B protease (A) (PDB ID: 2PC0 [13]), M36 appears to provide anchorage for E35, and stabilizes the salt bridge between E35 and R57.…”

Section: Effect Of Secondary Resistance Mutations On Flap Movementmentioning

confidence: 99%

“…Polymorphic sites of the subtype B protease (PDB ID: 2PC0) [13] and the C-SA protease (PDB ID: 3U71) [37]. The flexible flaps of the protease (residues at positions [46][47][48][49][50][51][52][53][54] are coloured cyan. The fulcrum region (residues at positions 10-23), hinge region (residues at positions 35-42 and 57-61) and cantilever region (residues at positions 62-78) are implicated in flap opening.…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Amide hydrogen exchange in HIV–1 subtype B and C proteases – insights into reduced drug susceptibility and dimer stability

et al. 2014

View full text Add to dashboard Cite

Since its identification, HIV has continued to have a detrimental impact on the lives of millions of people throughout the world. The protease of HIV is a major target in antiviral treatment. The South African HIV–1 subtype C (C–SA) protease displays weaker binding affinity for some clinically approved protease inhibitors in comparison with the HIV–1 subtype B protease. The heavy HIV burden in sub‐Saharan Africa, where subtype C HIV–1 predominates, makes this disparity a topic of great interest. In light of this, the enzyme activity and affinity of protease inhibitors for the subtype B and C–SA proteases were determined. The relative vitality, indicating the selective advantage of polymorphisms, of the C–SA protease relative to the subtype B protease in the presence of ritonavir and darunavir was four‐ and tenfold greater, respectively. Dynamic differences that contribute to the reduced drug susceptibility of the C–SA protease were investigated by performing hydrogen–deuterium exchange/mass spectrometry (HDX/MS) on unbound subtype B and C–SA proteases. The reduced propensity to form the E35–R57 salt bridge, and alterations in the hydrophobic core of the C–SA protease, are proposed to affect the anchoring of the flexible flaps, resulting in an increased proportion of the fully open flap conformation. HDX/MS data suggested that the N–terminus of both proteases is less stable than the C–terminus of the proteases, thus explaining the increased efficacy of dimerization inhibitors targeted toward the C–terminus of HIV proteases. As far as we are aware, this is the first report on assessment of HIV protease dynamics using HDX/MS.

show abstract

Section: Effect Of Secondary Resistance Mutations On Flap Movementmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Amide hydrogen exchange in HIV–1 subtype B and C proteases – insights into reduced drug susceptibility and dimer stability

et al. 2014

View full text Add to dashboard Cite

show abstract

“…The most frequent, L90M and others including G48V (9.0%) and I84V (7.1%) are contraindications to the use of saquinavir associated with ritonavir (SQV/r) (32)(33)(34). The mutations I84V (7.1%), V32I (4.0%), I47V (1.6%), and I54L (0.8%), are contraindications to the use of fosamprenavir associated with ritonavir (FSP/r) (35)(36)(37). The number of licensed PI antiretroviral drug class has expanded and the number of mutations associated with PI resistance is higher when compared with other antiretroviral drug classes.…”

Section: ------------------------------------------------------------mentioning

confidence: 99%

Frequency and diversity of human immunodeficiency virus type 1 mutations associated with antiretroviral resistance among patients from Southern Brazil failing highly active antiretroviral therapy (HAART)

Saad

Morimoto²,

Wiechmann³

et al. 2010

Int J Mol Med

View full text Add to dashboard Cite

Abstract. The human immunodeficiency virus type 1 (HIV-1) epidemic in Brazil is spreading to small municipalities as well as the innermost parts of the country and scarce information has been reported on the frequency of HIV-1 resistanceassociated mutations in these areas. To determine the frequency and diversity of the HIV-1 antiretroviral resistance-associated mutations among patients failing highly active antiretroviral therapy from Londrina in Southern Brazil, 127 HIV-1 genotyping tests that were assayed during January 2000 to July 2008 from 108 patients were evaluated. Sixty-nine patients (63.9%) were male and 39 (36.1%) were female and the age ranged from 10 to 68 years (mean, 40.8±9.2). All of them showed at least one HIV-1 antiretroviral resistance-associated mutation and in 72 (56.7%) genotyping tests, mutations for the three antiretroviral classes were detected simultaneously. Mutations associated with resistance to protease inhibitor (PI) were detected in 124 tests (97.6%), the main ones were L90M in 28 (22.0%), V82A in 27 (21.2%), M46I in 26 (20.5%), and I54V in 23 (18.1%). The main mutations associated with nucleoside reverse transcriptase inhibitor (NRTI) resistance were M184V in 82 (64.6%), and the thymidine analog mutations were D67N in 51 (40.1%) tests, K70R in 45 (35.4%), T215Y in 40 (31.5%), and M41L in 38 (30.0%). The most frequent major mutations associated with resistance to nonnucleoside RT inhibitors (NNRTI) were K103N in 47 (37.0%), G190A in 11 (8.7%), and G190S in 2 (2.6%) tests. Mutations associated with reduced susceptibility to NRTI and IP simultaneously were observed in 46 (36.2%) tests. The results obtained may contribute to the improvement of the treatment strategies and the management of the antiretroviral drug therapy of HIV-1-infected patients from this Brazilian region, reducing public costs for antiretroviral drugs which have not been efficient in therapy.

show abstract

“…The protease mutations selected in vitro or in vivo in the presence of amprenavir (I50V, V32I plus I47V, I54LM/M, and I84V) (13) are rarely selected in patients treated by first-line FPV-containing regimens, particularly when boosted with ritonavir (RTV) (12,22). In PIexperienced patients, few data are available concerning the prediction of virological response to FPV/r by genotypic resistance analysis (2,17,20). Recently, the ANRS proposed a genotypic interpretation algorithm for FPV/r including a genotypic score (L10F/I/V, L33F, M36I, I54L/M/V/A/T/S, I62V, V82A/F/C/G, I84V, and L90M) and the presence or absence of the mutations I50V or V32I plus I47V/A as an independent predictor of virological response in 73 PI-experienced patients (17).…”

Section: The Aim Of This Study Was To Identify Human Immunodeficiencymentioning

confidence: 99%

Genotypic Resistance Analysis of the Virological Response to Fosamprenavir-Ritonavir in Protease Inhibitor-Experienced Patients in CONTEXT and TRIAD Clinical Trials

Marcelin

Flandre

Molina

et al. 2008

Antimicrob Agents Chemother

View full text Add to dashboard Cite

The aim of this study was to identify human immunodeficiency virus (HIV؊11 ). In the nine patients with zero mutations within this set, the median decrease in HIV RNA was ؊2.63 log copies/ml, and was ؊2.22 (n ‫؍‬ 45), ؊1.50 (n ‫؍‬ 26), ؊0.58 (n ‫؍‬ 23), ؊0.47 (n ‫؍‬ 6), ؊0.13 (n ‫؍‬ 3), and 0.04 (n ‫؍‬ 1) log copies/ml in those with one, two, three, four, five, and six mutations, respectively. This study identified six mutations associated with VR to FPV/r. Some of these mutations are shared with the current FPV/r Agence Nationale de Recherches sur le SIDA (ANRS) resistance score, which has been cross-validated in the CONTEXT/TRIAD data set, suggesting that the current ANRS FPV/r score is a useful tool for the prediction of VR to FPV/r in PI-experienced patients.

show abstract

Interpretation of Genotype and Pharmacokinetics for Resistance to Fosamprenavir-Ritonavir-Based Regimens in Antiretroviral-Experienced Patients

Cited by 22 publications

References 34 publications

Amide hydrogen exchange in HIV–1 subtype B and C proteases – insights into reduced drug susceptibility and dimer stability

Amide hydrogen exchange in HIV–1 subtype B and C proteases – insights into reduced drug susceptibility and dimer stability

Frequency and diversity of human immunodeficiency virus type 1 mutations associated with antiretroviral resistance among patients from Southern Brazil failing highly active antiretroviral therapy (HAART)

Genotypic Resistance Analysis of the Virological Response to Fosamprenavir-Ritonavir in Protease Inhibitor-Experienced Patients in CONTEXT and TRIAD Clinical Trials

Contact Info

Product

Resources

About