2013
DOI: 10.1310/hct1405-216
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Efficacy and Safety 48 Weeks after Switching from Efavirenz to Rilpivirine Using Emtricitabine/Tenofovir Disoproxil Fumarate–Based Single-Tablet Regimens

Abstract: Switching from EFV/FTC/TDF to RPV/FTC/ TDF was a safe, efficacious option for virologically suppressed HIV-infected patients with EFV intolerance wishing to remain on an STR.

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Cited by 67 publications
(92 citation statements)
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“…For DOR, at a daily dose of 100 mg (the dose employed in the phase 3 clinical trials), the plasma trough concentration at 24 h is 830 nM. The trough concentrations of EFV and RPV are 5,600 nM and 260 nM at 24 h at clinical doses of 600 mg and 25 mg, respectively (18,19). These values and the respective IC 50 s determined in the presence of 100% serum were used to calculate IQs for each of these drugs versus the panel of NNRTI mutants, as shown in Fig.…”
Section: Resultsmentioning
confidence: 99%
“…For DOR, at a daily dose of 100 mg (the dose employed in the phase 3 clinical trials), the plasma trough concentration at 24 h is 830 nM. The trough concentrations of EFV and RPV are 5,600 nM and 260 nM at 24 h at clinical doses of 600 mg and 25 mg, respectively (18,19). These values and the respective IC 50 s determined in the presence of 100% serum were used to calculate IQs for each of these drugs versus the panel of NNRTI mutants, as shown in Fig.…”
Section: Resultsmentioning
confidence: 99%
“…Nell'ambito degli inibitori nucleosidici/nucleotidici della transcriptasi inversa (NRTI), i dati della letteratura hanno evidenziato generalmente una riduzione dei valori di trigliceridi, colesterolo totale ed LDL sostituendo stavudina, didanosina o zidovudina con tenofovir (preferibile) o abacavir (in alternativa, se il test HLA B*5701 è negativo) (24,25). Tra gli inibitori non nucleosidici della transcriptasi inversa (NNRTI), efavirenz è associato più spesso a dislipidemia e può essere sostituito, con effetti favorevoli sui parametri lipidici, da altri NNRTI (quali nevirapina, etravirina o rilpivirina) o da un inibitore dell'integrasi (raltegravir) (26)(27)(28)(29)(30). Gli inibitori della proteasi boosterati con ritonavir (PI/r) sono i farmaci più spesso associati a ipertrigliceridemia e/o ipercolesterolemia e gli studi di switch hanno dimostrato che si può ottenere un miglioramento significativo della dislipidemia sostituendo il PI/r con un altro PI a minor impatto sull'assetto lipidico (atazanavir, atazanavir/r, darunavir/r), con un NNRTI (nevirapina, etravirina, rilpivirina) o con un inibitore dell'integrasi (raltegravir, elvitegravir/cobicistat) (31-39).…”
Section: Gestione Del Rischio Cardiovascolare: Stile DI Vita E Terapiunclassified
“…Consistent with STaR, all patients in a smaller trial (Study 111; n = 49) who were already virologically suppressed with the emtricitabine/efavirenz/tenofovir DF single-tablet regimen, but wished to change their regimen because of efavirenz intolerance, sustained a viral load of \50 copies/mL 12 weeks after switching to the emtricitabine/rilpivirine/tenofovir DF single-tablet regimen [8,13] or full analysis set [11,12], using the time-to-loss-of-virological response [8,13] or snapshot [11,12] algorithm for virological outcomes BL baseline, EFV efavirenz, FTC emtricitabine, pts patients, RPV rilpivirine, TDF tenofovir disoproxil fumarate a Pts received FTC/RPV/TDF 200 mg/25 mg/300 mg or FTC/EFV/TDF 200 mg/600 mg/300 mg as once-daily single-tablet regimens in STaR, and RPV 25 mg or EFV 600 mg once daily in combination with FTC/TDF in ECHO and THRIVE b Primary endpoint at week 48 c 95 % confidence interval for the difference between the RPV group and comparator group d RPV regimen was noninferior to the EFV regimen, based on a noninferiority margin of 12 % for the between-regimen difference e Statistical analysis for between-group difference was not reported (primary endpoint), with most patients continuing to sustain this degree of suppression up to 48 weeks (Table 3) [30,31]. At 48 weeks, no significant change in CD4?…”
Section: How Is It Available?mentioning
confidence: 99%
“…cell count was evident and fewer than 5 % of patients experienced virological failure (Table 3). Most patients (92 %) were C95 % adherent through week 48, as measured by pill count [30].…”
Section: How Is It Available?mentioning
confidence: 99%
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