2015 Help me understand this report
RandomizEd phase II trial of Sunitinib four weeks on and two weeks off versus Two weeks on and One week off in metastatic clear-cell type REnal cell carcinoma: RESTORE trial
Abstract: Sunitinib administered with a 2/1 schedule is associated with less toxicity and higher FFS at 6 months than a 4/2 schedule, without compromising the efficacy in terms of ORR and TTP (NCT00570882).
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Cited by 101 publications
(99 citation statements)
References 16 publications
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“…[20][21][22][23][24] Three ongoing prospective studies (NCT02060370, NCT02689167, and NCT02398552) will further evaluate the value of the two/ one schedule. It is important to note that based on the dose/schedule distribution (Table 1) in our individualization study, the two/ one schedule was optimal in only 39 (37%) patients.…”
Section: Changing the Schedule From Four/two To Two/one May Not Optimmentioning
confidence: 99%
“…[20][21][22][23][24] Three ongoing prospective studies (NCT02060370, NCT02689167, and NCT02398552) will further evaluate the value of the two/ one schedule. It is important to note that based on the dose/schedule distribution (Table 1) in our individualization study, the two/ one schedule was optimal in only 39 (37%) patients.…”
Section: Changing the Schedule From Four/two To Two/one May Not Optimmentioning
confidence: 99%
“…9 The primary endpoint of failure-free survival (FFS) at six months was higher in the two/one schedule than in the four/two schedule (63% vs. 44%), as was FFS (7.6 months vs. 6.0 months; p=0.029). The two/one schedule was associated with less frequent treatment-emergent AEs, including stomatitis, rash, and hand-foot syndrome.…”
Section: Henry Jacob Conter MD Mscmentioning
confidence: 97%
“…Большин-ство опубликованных исследований посвящено сравнению режима 4 / 2 с режимом 2 / 1 (2 недели ежедневного прие-ма сунитиниба в дозировке 50 мг с последующим недель-ным перерывом). Был опубликован ряд ретроспективных исследований, в которых было показано преимущество в уменьшении частоты побочных явлений при назначении режима 2 / 1 над традиционным режимом 4 / 2 [14][15][16][17][18][19][20][21][22].…”
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“…В единственном опубликованном проспективном ис-следовании II фазы [20] пациенты с светлоклеточным мПКР были рандомизированы на получение терапии сунити-нибом по схеме 4 / 2 (n=36) и по схеме 2 / 1 (n=38). Пер-вичной целью исследования была 6-месячная выжива-емость без отмены лечения.…”
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