Changes in Human Immunodeficiency Virus Type 1 Populations after Treatment Interruption in Patients Failing Antiretroviral Therapy

Hance, Allan J.; Lemiale, Virginie; Izopet, Jacques; Lecossier, Denise; Joly, Véronique; Massip, Patrice; Mammano, Fabrizio; Descamps, Diane; Brun‐Vézinet, Françoise; Clavel, François

doi:10.1128/jvi.75.14.6410-6417.2001

Cited by 120 publications

(98 citation statements)

References 30 publications

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“…Even after up to 12 months of RTV treatment and in the presence of several pro mutations that could be considered compensatory in nature, none of the resistant variants recovered pretreatment-specific infectivity levels, consistent with observations made by others (2). The reversion of resistant virus populations to drug-susceptible populations even after prolonged treatment failure (Ն12 months) also suggests that compensation is indeed incomplete (15,18,24,30). The infectivity measurements presented here are consistent with the infectivity of single-, double-, and triple-mutant strains described by Mammano et al (37) but lower than the fitness of clones harboring multiple resistance mutations measured by coculture experiments (40,44).…”

Section: Discussionsupporting

confidence: 71%

Evolution of Human Immunodeficiency Virus Type 1 Protease Genotypes and Phenotypes In Vivo under Selective Pressure of the Protease Inhibitor Ritonavir

Resch¹,

Parkin

Watkins

et al. 2005

J Virol

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We examined the population dynamics of human immunodeficiency virus type 1 pro variants during the evolution of resistance to the protease inhibitor ritonavir (RTV) in vivo. pro variants were followed in subjects who had added RTV to their previously failed reverse transcriptase inhibitor therapy using a heteroduplex tracking assay designed to detect common resistance-associated mutations. In most cases the initial variant appeared rapidly within 2 to 3 months followed by one or more subsequent population turnovers. Some of the subsequent transitions between variants were rapid, and some were prolonged with the coexistence of multiple variants. In several cases variants without resistance mutations persisted despite the emergence of new variants with an increasing number of resistance-associated mutations. Based on the rate of turnover of pro variants in the RTV-treated subjects we estimated that the mean fitness of newly emerging variants was increased 1.2-fold (range, 1.02 to 1.8) relative to their predecessors. A subset of pro genes was introduced into infectious molecular clones. The corresponding viruses displayed impaired replication capacity and reduced susceptibility to RTV. A subset of these clones also showed increased susceptibility to two nonnucleoside reverse transcriptase inhibitors and the protease inhibitor saquinavir. Finally, a significant correlation between the reduced replication capacity and reduced processing at the gag NC-p1 processing site was noted. Our results reveal a complexity of patterns in the evolution of resistance to a protease inhibitor. In addition, these results suggest that selection for resistance to one protease inhibitor can have pleiotropic effects that can affect fitness and susceptibility to other drugs.Protease inhibitors (PIs) potently inhibit human immunodeficiency virus type 1 (HIV-1) replication, and their initial introduction into combination antiretroviral therapy was associated with a significant decrease of HIV-1-associated mortality and morbidity (41, 45). However, in clinical practice, virologic failure of protease inhibitor-containing therapy occurs in a significant fraction of the treated population (19,22,42,46,52,70). Virologic failure of protease inhibitor treatment is often due to the selection of HIV-1 strains with mutations in the pro gene, which encodes the viral protease (PR), and in specific protease cleavage sites encoded in the gag gene that collectively confer reduced drug susceptibility to the harboring strain (11,12,28,36,43,47,72).The resistance mutations are hypothesized to be largely preexisting, generated by the highly error-prone and rapid replication of HIV-1 in large virus populations (5, 10, 57). However, in PI-naïve subjects, some critical resistance mutations cannot be detected or can only be detected at very low levels, suggesting that these mutations may confer a selective disadvantage relative to wild-type HIV-1 strains (3,18,25,32,34,63). Indeed, it has been shown that the catalytic efficiency of protease is reduced by PI resis...

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Section: Discussionsupporting

confidence: 71%

Evolution of Human Immunodeficiency Virus Type 1 Protease Genotypes and Phenotypes In Vivo under Selective Pressure of the Protease Inhibitor Ritonavir

Resch¹,

Parkin

Watkins

et al. 2005

J Virol

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“…All plasma samples with a detectable viral load obtained during the interval between the initiation of treatment with protease inhibitors and the detection of L90M resistance mutation on standard genotyping were evaluated. The techniques used to quantify viral populations expressing the V82A and L90M mutations have previously been described (21). Briefly, 1 ml of plasma was centrifuged (23,500 ϫ g, 1 h, 4°C), and RNA was extracted from the pellet (QIAamp Viral RNA Mini Kit; Qiagen, Valencia, Calif.).…”

Section: Methodsmentioning

confidence: 99%

“…Although resistance mutations confer a decisive advantage to these variants over their parental wild-type counterparts for replication in the presence of antiretroviral drugs, there is accumulating evidence that resistant HIV strains are less fit than wild-type virus for replication in the absence of drug and that, overall, the replicative capacity of many drug-resistant HIV variants is reduced (1,2,4,7,13,19,21,22,37,39). Resistance mutations in the protease are thought to modify the size and shape of the substrate-binding domain of the enzyme, thereby reducing the affinity of inhibitors for the enzyme (30,39,44,47).…”

mentioning

confidence: 99%

“…It is now recognized that plasma virus is composed of a mixture of numerous quasispecies (8). In patients undergoing treatment and harboring resistant viral strains, the dominant quasispecies is accompanied by minority populations expressing distinct resistance genotypes (8,14,21,34,46). Because these viral species can evolve independently, an initially minority population, having followed a distinct evolutionary pathway, could emerge as the dominant population, either because it had evolved higher resistance or because a change in drug pressure gave that population a growth advantage over the prior majority population.…”

mentioning

confidence: 99%

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Role of Minority Populations of Human Immunodeficiency Virus Type 1 in the Evolution of Viral Resistance to Protease Inhibitors

Charpentier

Dwyer

Mammano

et al. 2004

J Virol

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Human immunodeficiency virus type 1 (HIV-1) drug resistance results from the accumulation of mutations in the viral genes targeted by the drugs. These genetic changes, however, are commonly detected and monitored by techniques that only take into account the dominant population of plasma virus. Because HIV-1-infected patients harbor a complex and diverse mixture of virus populations, the mechanisms underlying the emergence and the evolution of resistance are not fully elucidated. Using techniques that allow the quantification of resistance mutations in minority virus species, we have monitored the evolution of resistance in plasma virus populations from patients failing protease inhibitor treatment. Minority populations with distinct resistance genotypes were detected in all patients throughout the evolution of resistance. The emergence of new dominant genotypes followed two possible mechanisms: (i) emergence of a new mutation in a currently dominant genotype and (ii) emergence of a new genotype derived from a minority virus species. In most cases, these population changes were associated with an increase in resistance at the expense of a reduction in replication capacity. Our findings provide a preliminary indication that minority viral species, which evolve independently of the majority virus population, can eventually become dominant populations, thereby serving as a reservoir of diversity and possibly accelerating the development of drug resistance.

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“…[116][117][118][119][120] Unequal exposure to antiretrovirals and treatment interruptions are thought to underlie the development of resistance in some patients. [121][122][123][124][125] Different rates of adherence to medications within a regimen (discordant adherence) combined with varied pharmacokinetics of the agents can lead to viral replication, and subsequent exposure to sub-optimal treatment regimens. 77,98,126,127 Fixed-dose regimens such as Atripla may promote more complete adherence in a "take one, take all" fashion which would limit unequal viral exposure to cART components.…”

Section: Resistancementioning

confidence: 99%

Issues in resistance, adherence, and comparative efficacy of the single-tablet regimen combination of tenofovir, emtricitabine, and efavirenz in the management of HIV-1 infection

Rebick¹,

Walmsley²

2012

VAAT

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Abstract:Atripla is the first once-daily, single-tablet, triple-combination antiretroviral therapy. It is recommended for the initial treatment of the naïve patient with human immunodeficiency virus-1 (HIV-1) infection in all current guidelines, based on its proven efficacy in numerous head-to-head randomized clinical trials. Not only has it proven efficacy, but the fixed-dose combination, Atripla, has resulted in an improvement in adherence, quality of life, and satisfaction among naïve as well as virally suppressed patients switching from another regimen. Despite the advantages, tolerability issues can arise that are related primarily to the efavirenz component, which is known to cause central nervous side effects such as dizziness, abnormal dreams, and anxiety. Although generally self-limited, these side-effects can lead to treatment discontinuation in the short-or long-term. Based on the observation of neural tube defects in macaque models, and isolated case reports in human fetuses with first trimester exposure, it is rated as Food and Drug Administration pregnancy category D, and considered as contraindicated in the first trimester of pregnancy where alternatives are available. Given the low genetic barrier of each of the individual components, resistance remains an important issue for patients with poor adherence, but is balanced in part by the long half-life of the drugs. Transmitted resistance is described in up to 16% of newly infected patients in population surveys, and is particularly prevalent in men who have sex with men. Minority variants that may impart resistant to efavirenz are not detected with currently used HIV-1 genotype assays, but nonetheless may also be implicated in patients who fail initial treatment. Several single-tablet regimens are recently licensed or in development that will challenge Atripla as the single-tablet first-line option, but none have shown superior efficacy to date.

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Changes in Human Immunodeficiency Virus Type 1 Populations after Treatment Interruption in Patients Failing Antiretroviral Therapy

Cited by 120 publications

References 30 publications

Evolution of Human Immunodeficiency Virus Type 1 Protease Genotypes and Phenotypes In Vivo under Selective Pressure of the Protease Inhibitor Ritonavir

Evolution of Human Immunodeficiency Virus Type 1 Protease Genotypes and Phenotypes In Vivo under Selective Pressure of the Protease Inhibitor Ritonavir

Role of Minority Populations of Human Immunodeficiency Virus Type 1 in the Evolution of Viral Resistance to Protease Inhibitors

Issues in resistance, adherence, and comparative efficacy of the single-tablet regimen combination of tenofovir, emtricitabine, and efavirenz in the management of HIV-1 infection

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