TY - JOUR
T1 - Long-term safety and efficacy of benralizumab in patients with severe, uncontrolled asthma
T2 - 1-year results from the BORA phase 3 extension trial
AU - Busse, William W.
AU - Bleecker, Eugene R.
AU - FitzGerald, J. Mark
AU - Ferguson, Gary T.
AU - Barker, Peter
AU - Sproule, Stephanie
AU - Olsson, Richard F.
AU - Martin, Ubaldo J.
AU - Goldman, Mitchell
AU - BORA study investigators
AU - Yañez, Anahí
AU - Fernández, Marcelo
AU - Tolcachier, Alberto
AU - Belloni, Juan
AU - Taborda, Jorge
AU - De Salvo, Maria
AU - Maspero, Jorge
AU - Victorio, Carlos
AU - Navarta, Miguel Chirino
AU - Grilli, Monica
AU - Rodríguez, Pablo
AU - Otaola, María
AU - Cambursano, Víctor
AU - Malamud, Patricia
AU - Stok, Ana
AU - Arce, German
AU - Roza, Osiris
AU - Scherbovsky, Fernando
AU - Elias, Pedro
AU - Saez, Maria Salazan
AU - Peters, Matthew
AU - Phillips, Martin
AU - Upham, John
AU - Gibson, Peter
AU - Thien, Francis
AU - Douglass, Jo
AU - Thomas, Paul
AU - Bardin, Philip
AU - Sajkov, Dimitar
AU - Hew, Mark
AU - Langton, David
AU - Pez, Andreia
AU - Fritscher, Carlos
AU - Hetzel, Jorge
AU - Mattos, Waldo
AU - Stelmach, Rafael
AU - Antila, Martti
AU - Fernandes, Ana Luisa
AU - Metev, Hristo
AU - Ivanov, Yavor
AU - Bogdanova, Aneliya
AU - Markova, Ana Dancheva
AU - Peneva, Marinka
AU - Veselinova, Rumyana
AU - Petkova, Tatyana
AU - Petrova, Vanushka
AU - Shopova, Elena
AU - Ivanova, Yuliya
AU - Yotsova, Rumyana
AU - Kirkova, Ginka
AU - Petrova, Galina
AU - Dachev, Svetoslav
AU - Sotirova, Kostadinka
AU - Stoyanova, Mariyana
AU - Yakov, Oleg
AU - Ilieva-Fartunova, Vanya
AU - Lemiere, Catherine
AU - Laviolette, Michel
AU - Yang, William
AU - Pek, Bonavuth
AU - Killorn, William Patrick
AU - Poirier, Claude
AU - Chouinard, Guy
AU - Melenka, Lyle
AU - Leigh, Richard
AU - Nair, Parameswaran
AU - Dorscheid, Delbert
AU - Martin, James
AU - Pavie, Juana
AU - Rosenblut, Andres
AU - Cartagena, Claudia
AU - Quilodran, Carlos
AU - Muñoz, Silvia
AU - Malkusova, Ivana
AU - Veverka, Josef
AU - Holub, Stanislav
AU - Mares, Jaroslav
AU - Kozel, Radovan
AU - Kopecka, Daniela
AU - Zindr, Vladimir
AU - Cerva, Pavel
AU - Chanez, Pascal
AU - Bourdin, Arnaud
AU - Devouassoux, Gilles
AU - Taille, Camille
AU - De Blay, Frédéric
AU - Goupil, Francois
AU - Leroyer, Christophe
AU - Gourcerol, Delphine
AU - Didi, Toufik
AU - Didier, Alain
AU - Garcia, Gilles
AU - Bonniaud, Philippe
AU - Vasram, Riazate Rossanaly
AU - Lommatzsch, Marek
AU - Harnest, Ulf
AU - Linnhoff, Anneliese
AU - Keller, Claus
AU - Hoheisel, Gerhard
AU - Förster, Karin
AU - Schultz, Thomas
AU - Schenkenberger, Isabelle
AU - Kirschner, Joachim
AU - Schmoller, Tibor
AU - Zielen, Stefan
AU - Kornmann, Marc
AU - Beck, Ekkehard
AU - Volgmann, Lutz
AU - Dichmann, Rolf
AU - Overlack, Axel
AU - Winkler, Jörg
AU - Mikloweit, Petra
AU - Ballenberger, Sabine
AU - Rolke, Mathias
AU - Korn, Stephanie
AU - Pabel, Helmut
AU - Hoffmann, Martin
AU - Feimer, Jan
AU - Rabe, Klaus
AU - Deckelmann, Regina
AU - Welte, Tobias
AU - Ohbayashi, Hiroyuki
AU - Hozawa, Soichiro
AU - Shimoda, Terufumi
AU - Yoshida, Makoto
AU - Nagakura, Toshikazu
AU - Kamei, Tadashi
AU - Sano, Yasuyuki
AU - Kagami, Shinichiro
AU - Takahashi, Hisaho
AU - Haida, Michiko
AU - Kimura, Goro
AU - Nakamura, Hiroyuki
AU - To, Yasuo
AU - Shinkai, Masaharu
AU - Shimokawaji, Tadasuke
AU - Kudo, Makoto
AU - Shijyubo, Noriharu
AU - Tochigi, Takao
AU - Kato, Motokazu
AU - Tanaka, Akihiko
AU - Gon, Yasuhiro
AU - Sasaki, Norihisa
AU - Ohdaira, Tetsuro
AU - Omori, Chiharu
AU - Takahashi, Toshiki
AU - Takeuchi, Satomi
AU - Nakajima, Kiyotaka
AU - Makita, Hironi
AU - Kaneko, Masahiro
AU - Furuta, Kenjiro
AU - Taniguchi, Masami
AU - Inobe, Yoshito
AU - Miki, Hiroshi
AU - Nakamura, Yoichi
AU - Miyazawa, Naoki
AU - Yano, Shuichi
AU - Iijima, Masayuki
AU - Yamato, Tsuyoshi
AU - Diaz, Javier
AU - Matsuno, Alberto
AU - Felix, Efrain
AU - Guerreros, Alfredo
AU - Daly, Alejandro
AU - Rodriguez Chariarse, Fernando
AU - Salazar, Danilo
AU - Castro, Socorro
AU - Chavez, William
AU - Estrella, Rolando
AU - Aquino, Teresita
AU - Atienza, Tito
AU - Samoro, Ronnie
AU - Isidro, Marie Grace Dawn
AU - Kuna, Piotr
AU - Antczak, Adam
AU - Bednarek, Michał
AU - Mądra-Rogacka, Danuta
AU - Hofman, Teresa
AU - Jutel, Marek
AU - Pisarczyk-Bogacka, Ewa
AU - Kot, Agata
AU - Mróz, Robert
AU - Czupryńska-Borkowska, Małgorzata
AU - Żurowska-Gębala, Małgorzata
AU - Dyczek, Andrzej
AU - Jasieniak-Pinis, Grażyna
AU - Wojnowski, Piotr
AU - Trębas-Pietraś, Ewa
AU - Dobryniewska, Małgorzata
AU - Stobiecki, Marcin
AU - Tarnowska-Matusiak, Marzenna
AU - Magner, Alina
AU - Kolczyński, Andrzej
AU - Kachel, Tomasz
AU - Bartuzi, Zbigniew
AU - Majorek-Olechowska, Bernadetta
AU - Śliwiński, Paweł
AU - Balicka, Violetta
AU - Hajoł, Elżbieta
AU - Stachera, Jacek
AU - Rachel, Marta
AU - Michnar, Marek
AU - Tałałaj, Jarosław
AU - Springer, Ewa
AU - Napora, Piotr
AU - Grzelewski, Tomasz
AU - Bijata-Bronisz, Renata
AU - Świderska, Anna
AU - Mincewicz, Grzegorz
AU - Sankowski, Zbigniew
AU - Fijołek, Tomasz
AU - Kwaśniewski, Artur
AU - Jerzyńska, Joanna
AU - Cygler, Jerzy
AU - Olesiejuk, Ryszard
AU - Von Steiner, Iwona
AU - Machowiak, Wojciech
AU - Filipek, Krzysztof
AU - Piskorz, Piotr
AU - Uhryn, Ewa
AU - Nittner-Marszalska, Marita
AU - Rybicka-Liszewska, Elżbieta
AU - Bodzenta-Łukaszyk, Anna
AU - Chełmińska, Marta
AU - Krupa-Borek, Izabella
AU - Skucha, Wojciech
AU - Płoszczuk, Anna
AU - Mihaescu, Traian
AU - Petrui, Ioan Dorin
AU - Lee, Sang Pyo
AU - Lee, Byung Jae
AU - Lee, Sook Young
AU - Kim, Hee Kyoo
AU - Scott, Stephen
AU - Shaikh, Zeeshan
AU - Campbell, Edward
AU - Wong, Stephen
AU - Johnston, Janice
AU - Johnson, Thomas
PY - 2019/1/1
Y1 - 2019/1/1
N2 - Background: Benralizumab is an interleukin-5 receptor α-directed cytolytic monoclonal antibody that has been shown to safely reduce exacerbations and improve lung function for patients with asthma. We assessed the long-term safety and efficacy of benralizumab for patients with severe, uncontrolled eosinophilic asthma. Methods: We conducted a randomised, double-blind, parallel-group, phase 3 extension study at 447 sites in 24 countries. Eligible patients had to have completed the SIROCCO or CALIMA trials and remained on subcutaneous benralizumab 30 mg every 4 weeks (Q4W) or every 8 weeks (Q8W). Patients who had received placebo in those trials were re-randomised in a 1:1 ratio, using an interactive web-based system, to benralizumab 30 mg either Q4W or Q8W (first three doses 4 weeks apart). Treatment lasted for 56 weeks for adult patients (age ≥18 years) and 108 weeks for adolescent patients (age 12–17 years). The primary endpoint was the safety and tolerability of the two dosing regimens of benralizumab up to 68 weeks for adult patients (including the follow-up visit post-treatment) and up to 56 weeks for adolescent patients. This endpoint was assessed in the full analysis set, which included all patients from the SIROCCO and CALIMA predecessor studies who received at least one dose of study treatment in BORA and did not continue into another trial. This study is registered with ClinicalTrials.gov (NCT02258542). Findings: Between Nov 19, 2014, and July 6, 2016, we enrolled 1926 patients, of whom 633 had received benralizumab Q4W and 639 had received benralizumab Q8W in SIROCCO or CALIMA. The remaining 654 patients had received placebo in those trials and were randomly re-assigned in this trial to receive benralizumab Q4W (n=320) or Q8W (n=334). 1576 patients, including 783 who received benralizumab Q4W (265 newly assigned) and 793 who received benralizumab Q8W (281 newly assigned), were included in the full analysis set. The most common adverse events in all groups were viral upper respiratory tract infection (14–16%) and worsening asthma (7–10%). The most common serious adverse events were worsening asthma (3–4%), pneumonia (<1% to 1%), and pneumonia caused by bacterial infection (0–1%). The percentages of patients who had any on-treatment adverse event, any serious adverse event, or any adverse event leading to treatment discontinuation during BORA were similar between patients originally assigned benralizumab and those originally assigned placebo and between benralizumab treatment regimens. The percentage of patients who had any adverse event was similar between SIROCCO or CALIMA (71–75%; benralizumab group only) and BORA (65–71%), as was the percentage of patients who had an adverse event that led to treatment discontinuation (2% in SIROCCO and CALIMA vs 2–3% in BORA). Interpretation: The 2 years of safety results validate that observations observed in the first year of benralizumab continued through a second year of treatment. No new consequences of long-term eosinophil depletion occurred, and the incidence of other adverse events, including opportunistic infections, were similar during the second year. Funding: AstraZeneca and Kyowa Hakko Kirin.
AB - Background: Benralizumab is an interleukin-5 receptor α-directed cytolytic monoclonal antibody that has been shown to safely reduce exacerbations and improve lung function for patients with asthma. We assessed the long-term safety and efficacy of benralizumab for patients with severe, uncontrolled eosinophilic asthma. Methods: We conducted a randomised, double-blind, parallel-group, phase 3 extension study at 447 sites in 24 countries. Eligible patients had to have completed the SIROCCO or CALIMA trials and remained on subcutaneous benralizumab 30 mg every 4 weeks (Q4W) or every 8 weeks (Q8W). Patients who had received placebo in those trials were re-randomised in a 1:1 ratio, using an interactive web-based system, to benralizumab 30 mg either Q4W or Q8W (first three doses 4 weeks apart). Treatment lasted for 56 weeks for adult patients (age ≥18 years) and 108 weeks for adolescent patients (age 12–17 years). The primary endpoint was the safety and tolerability of the two dosing regimens of benralizumab up to 68 weeks for adult patients (including the follow-up visit post-treatment) and up to 56 weeks for adolescent patients. This endpoint was assessed in the full analysis set, which included all patients from the SIROCCO and CALIMA predecessor studies who received at least one dose of study treatment in BORA and did not continue into another trial. This study is registered with ClinicalTrials.gov (NCT02258542). Findings: Between Nov 19, 2014, and July 6, 2016, we enrolled 1926 patients, of whom 633 had received benralizumab Q4W and 639 had received benralizumab Q8W in SIROCCO or CALIMA. The remaining 654 patients had received placebo in those trials and were randomly re-assigned in this trial to receive benralizumab Q4W (n=320) or Q8W (n=334). 1576 patients, including 783 who received benralizumab Q4W (265 newly assigned) and 793 who received benralizumab Q8W (281 newly assigned), were included in the full analysis set. The most common adverse events in all groups were viral upper respiratory tract infection (14–16%) and worsening asthma (7–10%). The most common serious adverse events were worsening asthma (3–4%), pneumonia (<1% to 1%), and pneumonia caused by bacterial infection (0–1%). The percentages of patients who had any on-treatment adverse event, any serious adverse event, or any adverse event leading to treatment discontinuation during BORA were similar between patients originally assigned benralizumab and those originally assigned placebo and between benralizumab treatment regimens. The percentage of patients who had any adverse event was similar between SIROCCO or CALIMA (71–75%; benralizumab group only) and BORA (65–71%), as was the percentage of patients who had an adverse event that led to treatment discontinuation (2% in SIROCCO and CALIMA vs 2–3% in BORA). Interpretation: The 2 years of safety results validate that observations observed in the first year of benralizumab continued through a second year of treatment. No new consequences of long-term eosinophil depletion occurred, and the incidence of other adverse events, including opportunistic infections, were similar during the second year. Funding: AstraZeneca and Kyowa Hakko Kirin.
UR - http://www.scopus.com/inward/record.url?scp=85056170947&partnerID=8YFLogxK
U2 - 10.1016/S2213-2600(18)30406-5
DO - 10.1016/S2213-2600(18)30406-5
M3 - Article
C2 - 30416083
AN - SCOPUS:85056170947
SN - 2213-2600
VL - 7
SP - 46
EP - 59
JO - The Lancet Respiratory Medicine
JF - The Lancet Respiratory Medicine
IS - 1
ER -