TY - JOUR
T1 - Effect of double dose oseltamivir on clinical and virological outcomes in children and adults admitted to hospital with severe influenza: double blind randomised controlled trial
AU - AUTHOR GROUP
AU - Sedyaningsih, Endang Rahayu
AU - Malik, Moh Suhud
AU - Setiawaty, Vivi
AU - Trihono, Trihono
AU - Burhan, Erlina
AU - Aditama, Tjandra Yoga
AU - Soepandi, Prijanti Z.
AU - Partakusuma, Lia G.
AU - Sutiyoso, Agung P.
AU - Priatni, Ika
AU - Bandung, Rumah Sakit Hasan Sadikan
AU - Jusuf, Hadi
AU - Pranggono, Emmy Hermiyanti
AU - Soeroto, Arto Yuwono
AU - Setiabudi, Djatnika
AU - Somasetia, Dadang Hudaya
AU - Sudarwati, Sri
AU - Maskoen, Tini T.
AU - Hartantri, Yovita
AU - Parwati, Ida
AU - Giriputro, Sardikin
AU - Murniati, Dewi
AU - Sirait, Sondang Maryutka
AU - Soetanto, Tony
AU - Sulastri, Sri
AU - Agus, Rismali
AU - Rusli, Adria
AU - Wiweka, Sila
AU - Wignall, Steve
AU - Baird, Kevin
AU - Safika, Iko
AU - Sangsajja, Chariya
AU - Manosuthi, Weerawat
AU - Sutha, Patama
AU - Chuchottaworn, Chareon
AU - Sansayunh, Piamlarp
AU - Bangpattanasiri, Kittima
AU - Taylor, Walter R. J.
AU - Stepniewska, Kasia
AU - Fukuda, Caroline
AU - Lindegardh, Niklas
AU - White, Nicholas
AU - Day, Nick
AU - Chotpitayasunondh, Tawee
AU - Suntarattiwong, Piyarat
AU - Chantbuddhiwet, Umaporn
AU - Netsawang, Supichaya
AU - Chokephaibulkit, Kulkanya
AU - Vanprapar, Nirun
AU - de Jong, Menno D.
PY - 2013
Y1 - 2013
N2 - To investigate the validity of recommendations in treatment guidelines to use higher than approved doses of oseltamivir in patients with severe influenza. Double blind randomised trial. Thirteen hospitals in Indonesia, Singapore, Thailand, and Vietnam. Patients aged ≥ 1 year admitted to hospital with confirmed severe influenza. Oral oseltamivir at double dose (150 mg twice a day/paediatric equivalent) versus standard dose (75 mg twice a day/paediatric equivalent). Viral status according to reverse transcriptase polymerase chain reaction (RT-PCR) for influenza RNA in nasal and throat swabs on day five. Of 326 patients (including 246 (75.5%) children aged <15), 165 and 161 were randomised to double or standard dose oseltamivir, respectively. Of these, 260 (79.8%) were infected with influenza virus A (133 (40.8%) with A/H3N2, 72 (22.1%) with A/H1N1-pdm09, 38 (11.7%) with seasonal A/H1N1, 17 (5.2%) with A/H5N1) and 53 (16.2%) with influenza virus B. A further 3.9% (13) were false positive by rapid antigen test (negative by RT-PCR and no rise in convalescent haemagglutination inhibition titers). Similar proportions of patients were negative for RT-PCR on day five of treatment: 115/159 (72.3%, 95% confidence interval 64.9% to 78.7%) double dose recipients versus 105/154 (68.2%, 60.5% to 75.0%) standard dose recipients; difference 4.2% (-5.9 to 14.2); P=0.42. No differences were found in clearance of virus in subgroup analyses by virus type/subtype, age, and duration of illness before randomisation. Mortality was similar: 12/165 (7.3%, 4.2% to 12.3%) in double dose recipients versus 9/161 (5.6%, 3.0% to 10.3%) in standard dose recipients. No differences were found between double and standard dose arms in median days on supplemental oxygen (3 (interquartile range 2-5) v 3.5 (2-7)), in intensive care (4.5 (3-6) v 5 (2-11), and on mechanical ventilation (2.5 (1-16) v 8 (1-16)), respectively. No important differences in tolerability were found. There were no virological or clinical advantages with double dose oseltamivir compared with standard dose in patients with severe influenza admitted to hospital. Clinical Trials NCT00298233
AB - To investigate the validity of recommendations in treatment guidelines to use higher than approved doses of oseltamivir in patients with severe influenza. Double blind randomised trial. Thirteen hospitals in Indonesia, Singapore, Thailand, and Vietnam. Patients aged ≥ 1 year admitted to hospital with confirmed severe influenza. Oral oseltamivir at double dose (150 mg twice a day/paediatric equivalent) versus standard dose (75 mg twice a day/paediatric equivalent). Viral status according to reverse transcriptase polymerase chain reaction (RT-PCR) for influenza RNA in nasal and throat swabs on day five. Of 326 patients (including 246 (75.5%) children aged <15), 165 and 161 were randomised to double or standard dose oseltamivir, respectively. Of these, 260 (79.8%) were infected with influenza virus A (133 (40.8%) with A/H3N2, 72 (22.1%) with A/H1N1-pdm09, 38 (11.7%) with seasonal A/H1N1, 17 (5.2%) with A/H5N1) and 53 (16.2%) with influenza virus B. A further 3.9% (13) were false positive by rapid antigen test (negative by RT-PCR and no rise in convalescent haemagglutination inhibition titers). Similar proportions of patients were negative for RT-PCR on day five of treatment: 115/159 (72.3%, 95% confidence interval 64.9% to 78.7%) double dose recipients versus 105/154 (68.2%, 60.5% to 75.0%) standard dose recipients; difference 4.2% (-5.9 to 14.2); P=0.42. No differences were found in clearance of virus in subgroup analyses by virus type/subtype, age, and duration of illness before randomisation. Mortality was similar: 12/165 (7.3%, 4.2% to 12.3%) in double dose recipients versus 9/161 (5.6%, 3.0% to 10.3%) in standard dose recipients. No differences were found between double and standard dose arms in median days on supplemental oxygen (3 (interquartile range 2-5) v 3.5 (2-7)), in intensive care (4.5 (3-6) v 5 (2-11), and on mechanical ventilation (2.5 (1-16) v 8 (1-16)), respectively. No important differences in tolerability were found. There were no virological or clinical advantages with double dose oseltamivir compared with standard dose in patients with severe influenza admitted to hospital. Clinical Trials NCT00298233
U2 - https://doi.org/10.1136/bmj.f3039
DO - https://doi.org/10.1136/bmj.f3039
M3 - Article
C2 - 23723457
SN - 0959-8138
VL - 346
SP - f3039
JO - BMJ (Clinical research ed.)
JF - BMJ (Clinical research ed.)
ER -