Fenebrutinib Versus Placebo or Adalimumab in Rheumatoid Arthritis: A Randomized, Double‐Blind, Phase II Trial

Stanley Cohen,Katie Tuckwell,Tamiko R. Katsumoto,Rui Zhao,Joshua Galanter,Chin Lee,Julie Rae,Balázs Tóth,Nandhini Ramamoorthi,Jason A. Hackney,Alberto Berman,Nemanja Damjanov,Dmytro Fedkov,Sławomir Jeka,Leslie W. Chinn,Michael J. Townsend,Alyssa Morimoto,Mark C. Genovese,Alberto Berman, Alejandro Porto,Amelia Granel,C. Asnal,Eduardo Mysler, Gladys Alicia Testa,José Luis Velasco Zamora, José Moreno, Juan Pablo Gulin,Julio Hofman,María Rosa Ulla,Mirtha Sabelli, Pablo Alejandro Mannucci,Pablo Maid, Ana Cláudia Cauceglia Melazzi,Antônio Scafuto Scotton,Antônio Carlos Ximenes, E Funes,Emerson Alves Gimenez, Flora Maria D’Andrea Marcolino,João Francisco Marques Neto,Mauro Waldemar Keiserman,Sebastião Cézar Radominski,Sônia Maria Alvarenga Anti Loduca Lima, Thaís Rohde Pavan,Valderílio Feijó Azevedo, Aneliya Koleva,А. Toncheva,Daniela Bichovska,Delina Ivanova, Dimitar P Penev, Еmil Dimitrov,Mariyana Mihaylova, Nadezhda Kapandjieva, Natalia Marinova, Tanya Aleksieva,Tanya Tsvetanova, Tsvetanka Petranova, Валентина Попова,Yuliy A Spasov,Carlos Toro, Carlos Ernesto Arteaga Unigarro,Edwin Jáuregui,Javier Darío Márquez Hernández, Juan José Jaller Raad, Patricia Julieta Velez Sanchez,Chang Keun Lee,Chang‐Hee Suh,Eun Young Lee, Sang‐Heon Lee,Seong Wook Kang,Shin‐Seok Lee,Yun Jong Lee, Beatriz Elena Zazueta Montiel, Blanca Irma Pinzon de la O,Daniel Xibillé Friedmann, Francisco Rosas Lopez, Isaura Rodriguez Torres, Luis Jara Quezada,Marco Maradiaga Ceceña, Miguel Cortes Hernandez, Miguel Saavedra Salinas,Agnieszka Rapa,Agnieszka Pawtel,Agnieszka Zielińska,Anna Dudek, Anna Rizzi,Anna Strzelecka,Artur Racewicz,Barbara Stasiuk,Katarzyna Gruszecka,Krystyna Dworak,Sławomir Jeka, Tomasz Löwenhoff,A. Maslyanskiy,А. П. Ребров,Д. Г. Кречикова,Е С Жугрова,Е. Шмидт, Galina Matsievskaya,И. Б. Виноградова,Irina Ler,Larisa Eliseeva,L V Savina,Marina Stanislav,Mikhail Sandin,Natalia Zyablova,Н. И. Коршунов,Nino Mosesova, O. A. Polovnikova,O. B. Nesmeyanova,Р. Р. Самигуллина, Sergey Moiseev, С М Носков,Т. А. Раскина,Т. А. Попова,Valeriy N. Marchenko, Aleksandar Jovanovski,Bojana Stamenković,Gorica Ristić,M. Lazarevic,Mirjana Veselinović,Nada Vujasinović-Stupar,Nemanja Damjanov,Predrag Ostojić,A. Yagensky,A. Gnylorybov,Д. Г. Рекалов, Dmytroo Reshotko,Dmytro Fedkov, G. V. Dzyak, I. Gasanov,Л. Хіміон,Mykola Stanislavchuk, N. P. Prykhodko,Oleg Nadashkevych,Oleg P. Bortkevych,Orest Abrahamovych,Roman Yatsyshyn,Samvel Turyanytsya,Svitlana Smiyan,Vadym Vizir,V. Kachur,Vira Tseluyko,Vladyslav Povoroznyuk,В. І. Кошля,В. М. Ждан, Yurii Lymar,Yuriy Mostovoy,Angela Hawkes, Arthur R. Mabaquiao,Cong‐Qiu Chu, Craig D. Scoville, David Wyatt, D. Weinstein,Harris H. McIlwain, Jacqueline B Vo,Jeffrey Poiley,Joseph Z. Forstot,Kathryn H. Dao, Mark S. Turner,Mark C. Genovese,Michael Borofsky,Paul H. Caldron, Philip A Waller,Robert W. Levin,Samy Metyas, Scott Stein,Sharukh D. Shroff, Shirley Pang,Stanley Cohen, Tauseef Syed,Vishala Chindalore

Arthritis & Rheumatology（2020）

Cited 28|Views32

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Abstract

Objective To evaluate fenebrutinib, an oral and highly selective noncovalent inhibitor of Bruton's tyrosine kinase ( BTK ), in patients with active rheumatoid arthritis ( RA ). Methods Patients with RA and an inadequate response to methotrexate ( MTX ) (cohort 1; n = 480) were randomized to receive fenebrutinib (50 mg once daily, 150 mg once daily, or 200 mg twice daily), adalimumab (40 mg every other week), or placebo. Patients with RA and an inadequate response to tumor necrosis factor inhibitors (cohort 2; n = 98) received fenebrutinib (200 mg twice daily) or placebo. Both cohorts continued MTX therapy. Results In cohort 1, the percentages of patients in whom American College of Rheumatology 50% improvement criteria ( ACR 50) was achieved at week 12 were similar in the fenebrutinib 50 mg once daily and placebo groups, and were higher in the fenebrutinib 150 mg once daily group (28%) and 200 mg twice daily group (35%) than in the placebo group (15%) ( P = 0.016 and P = 0.0003, respectively). Fenebrutinib 200 mg twice daily and adalimumab (36%) were comparable ( P = 0.81). In cohort 2, ACR 50 was achieved in more patients receiving fenebrutinib 200 mg twice daily (25%) than placebo (12%) ( P = 0.072). The most common adverse events in the fenebrutinib groups included nausea, headache, anemia, and upper respiratory tract infections. Fenebrutinib had significant effects on myeloid and B cell biomarkers ( CCL 4 and rheumatoid factor). Fenebrutinib and adalimumab caused overlapping as well as distinct changes in B cell and myeloid biomarkers. Conclusion Fenebrutinib demonstrates efficacy comparable to adalimumab in patients with an inadequate response to MTX , and safety consistent with existing immunomodulatory therapies for RA . These data support targeting both B and myeloid cells via this novel mechanism for potential efficacy in the treatment of RA .

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Key words

fenebrutinib versus placebo,rheumatoid arthritis,adalimumab

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