2006
DOI: 10.1097/01.qai.0000234083.34161.55
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Rapid Emergence of Enfuvirtide Resistance in HIV-1-Infected Patients

Abstract: The rapid emergence of mutations associated with T-20 resistance in the absence of a fully suppressive antiretroviral regimen demonstrates a low genetic barrier to resistance and underscores the importance of combining T-20 with other active drugs when constructing regimens for highly treatment-experienced patients.

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Cited by 100 publications
(87 citation statements)
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“…ENF prevents this interaction and so provides a strong selective pressure for mutations in its binding site in the HR-1 domain (5, 10). However, mutations in HR-1 that prevent ENF binding are likely to impact the binding of the HR-2 domain as well, reducing the efficiency of membrane fusion (9,12,15,18,20,22,27,29,30,32). Indeed, when mutations that confer ENF resistance (19) are introduced into HR-1, membrane fusion kinetics are delayed, there is enhanced sensitivity to neutralizing antibodies that bind to the membrane-proximal region in gp41 (28), and virus fitness is reduced as measured by in vitro assays (19).…”
Section: Discussionmentioning
confidence: 99%
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“…ENF prevents this interaction and so provides a strong selective pressure for mutations in its binding site in the HR-1 domain (5, 10). However, mutations in HR-1 that prevent ENF binding are likely to impact the binding of the HR-2 domain as well, reducing the efficiency of membrane fusion (9,12,15,18,20,22,27,29,30,32). Indeed, when mutations that confer ENF resistance (19) are introduced into HR-1, membrane fusion kinetics are delayed, there is enhanced sensitivity to neutralizing antibodies that bind to the membrane-proximal region in gp41 (28), and virus fitness is reduced as measured by in vitro assays (19).…”
Section: Discussionmentioning
confidence: 99%
“…Resistance to ENF results mostly or entirely from mutations in the ENF binding site in the HR-1 region of gp41 (9,12,15,18,20,22,29,30,32). In a previous report, we characterized Env proteins derived from five treatment-experienced patients prior to ENF treatment and at a time on treatment after virologic failure (27).…”
Section: Hr-2 Mutations Compensate For the Hr-1-induced Delay In Fusimentioning
confidence: 99%
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“…Enfuvirtide, however, is administered subcutaneously -in contrast to other antiretroviral drugs, which are administered orally -and can cause significant injection site reactions (Oldfield et al, 2005). Further, resistance to enfuvirtide may emerge rapidly in patients, but may be reversed upon cessation of enfuvirtide administration (Lu et al, 2006;Poveda et al, 2005). It is of importance, therefore, to identify treatment protocols that maximize enfuvirtide efficacy and/or minimize enfuvirtide-related side-effects.…”
Section: Introductionmentioning
confidence: 99%
“…Enfurvirtide has antiviral activity similar to most other classes of antiretroviral drugs discussed above; however resistance develop rapidly in patients receiving the drug for salvage therapy who do not receive a sufficient number of RTI, PI and INI drugs such as efavirenz, lopinanir/r and raltegravir, respectively. The emergence of enfurvirtide resistant strains followed by virologic rebound has been observed in some patients within two to four weeks (Cabrera et al, 2006;Lu et al, 2006).…”
Section: Point Mutations Associated With Resistance To Fusion Inhibitorsmentioning
confidence: 99%