Safety and efficacy of rilzabrutinib vs placebo in adults with immune thrombocytopenia: the phase 3 LUNA3 study.

Mar 17, 2025

Experts: David J Kuter,Waleed Ghanima,Nichola Cooper,Howard Allen Liebman,Lei Zhang,Yu Hu,Yoshitaka Miyakawa,Wojciech Homenda,Luisa Elena Elena Morales Galindo,Ana Lisa Basquiera,Chuen Wen Tan,Guray Saydam,Marie Luise Hütter-Krönke,Chatree Chai-Adisaksopha,David Gomez-Almaguer,Huy Tran,Ho-Jin Shin,Ademar Dantas da Cunha Junior,Zsolt Lazar,Cristina Pascual-Izquierdo,Ilya Kirgner,Elisa Lucchini,Ganna Kuzmina,Michael Fillitz,Sylvain Audia,Minakshi Taparia,Matias Cordoba,Remco Diab,Mengjie Yao,Imene Gouia,Michelle Lee,Ahmed Abd Almalik Daak

Rilzabrutinib is a covalent, reversible BTK inhibitor with multiple mechanisms targeting key immune thrombocytopenia (ITP) disease pathophysiology. The phase 3 LUNA3 study in previously treated adults with persistent/chronic ITP evaluated oral rilzabrutinib 400 mg bid (n=133) vs placebo (n=69) for 24 weeks. At baseline overall, median age was 47 years (range, 18-80), 63% female, 7.7 year (range, 0.3-52.2) median duration of ITP, and 28% were splenectomized. Overall (N=202), 85 (64%) rilzabrutinib and 22 (32%) placebo patients achieved platelet response (≥50×109/L or 30×109/L-<50×109/L and doubled from baseline) during the first 12 weeks and were eligible to complete the double-blind period. The primary endpoint durable platelet response (platelet count ≥50×109/L for ≥two-thirds of ≥8 of the last 12 of 24 weeks without rescue therapy) was observed in 31 (23%) rilzabrutinib vs 0 placebo patients (P<0.0001). All secondary efficacy endpoints were significantly superior for rilzabrutinib (P<0.05). Median time to first platelet response was 15 d in rilzabrutinib responders. Rilzabrutinib significantly reduced rescue therapy use by 52% (P=0.0007) and improved week 25 bleeding scores (P=0.0006). Improved physical fatigue was sustained from week 13 (P=0.01) through 25 (P=0.0003). Treatment-related adverse events were mainly grade 1-2. One rilzabrutinib patient with multiple risk factors had serious treatment-related grade 3 peripheral embolism (lower left leg) and another died from unrelated pneumonia. Rilzabrutinib– in ITP patients who failed multiple previous therapies (splenectomy, TPO-RA, rituximab and/or fostamatinib) resulted in rapid and durable platelet response, reduced rescue medication use and bleeding, significantly improved physical fatigue, and showed favorable safety. NCT04562766; EudraCT 2020-002063-60.
Copyright © 2025 American Society of Hematology.

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ABOUT THE EXPERTS

David J Kuter,Waleed Ghanima,Nichola Cooper,Howard Allen Liebman,Lei Zhang,Yu Hu,Yoshitaka Miyakawa,Wojciech Homenda,Luisa Elena Elena Morales Galindo,Ana Lisa Basquiera,Chuen Wen Tan,Guray Saydam,Marie Luise Hütter-Krönke,Chatree Chai-Adisaksopha,David Gomez-Almaguer,Huy Tran,Ho-Jin Shin,Ademar Dantas da Cunha Junior,Zsolt Lazar,Cristina Pascual-Izquierdo,Ilya Kirgner,Elisa Lucchini,Ganna Kuzmina,Michael Fillitz,Sylvain Audia,Minakshi Taparia,Matias Cordoba,Remco Diab,Mengjie Yao,Imene Gouia,Michelle Lee,Ahmed Abd Almalik Daak

David J Kuter

Massachusetts General Hospital, Harvard Medical School, Boston, Massachusetts, United States.

Waleed Ghanima

Østfold Hospital, Grålum, Norway.

Nichola Cooper

Centre for Haematology, Department of Immunology and Inflammation, Imperial College London, London, United Kingdom, London, United Kingdom.

Howard Allen Liebman

University of Southern California, Los Angeles, California, United States.

Lei Zhang

Chinese Academy of Medical Sciences, Tianjn, China.

Yu Hu

Wuhan Xie’he Hospital, China.

Yoshitaka Miyakawa

Saitama Medical University Hospital, Saitama, Japan.

Wojciech Homenda

Regional Hospital, Slupsk and Institute of Health Sciences, Pomeranian University of Slupsk, Poland.

Luisa Elena Elena Morales Galindo

IC La Serena Research SpA, La Serena, Chile.

Ana Lisa Basquiera

Hospital Privado Universitario de Córdoba-Instituto Universitario de Ciencias Biomédicas de Córdoba (IUCBC), Cordoba, Argentina.

Chuen Wen Tan

Singapore General Hospital, Singapore, Singapore.

Guray Saydam

Ege University Medical Faculty, Izmir, Turkey.

Marie Luise Hütter-Krönke

Charité University medicine, Berlin, Germany.

Chatree Chai-Adisaksopha

Chiang Mai University, Chiang Mai, Thailand.

David Gomez-Almaguer

Hospital Universitario ¨Dr Jose Eleuterio Gonzalez¨, Monterrey, Mexico.

Huy Tran

Peninsula Private Hospital, Australia.

Ho-Jin Shin

Pusan National University Hospital, Busan, Korea, Republic of.

Ademar Dantas da Cunha Junior

Hospital do Cancer de Cascavel – UOPECCAN (Uniao Oeste Paranaense de Estudos e Combate ao Cancer), Cascavel, Brazil.

Zsolt Lazar

Petz Aladár University Teaching Hospital, Győr, Hungary.

Cristina Pascual-Izquierdo

Hospital General Universistario Gregorio Marañon, Madrid, Spain.

Ilya Kirgner

Tel Aviv Sourasky Medical.

Elisa Lucchini

Azienda Sanitaria Universitaria Giuliano Isontina, Trieste, Italy.

Ganna Kuzmina

Municipal Enterprise Kryvyi Rih City Clinical Hospital #2 of Kryvyi Rih City Council, SI Dnipropetrovsk Medical Academy under the Ministry of Health of Ukraine, Kryvyi Rih, Ukraine.

Michael Fillitz

Hanusch Hospital Vienna, Vienna, Austria.

Sylvain Audia

Department of Internal Medicine, University hospital of Dijon, University of Burgundy – Francois Mitterrand Hospital, France.

Minakshi Taparia

University of Alberta, Edmonton, Canada.

Matias Cordoba

Sanofi, Cambridge, Massachusetts, United States.

Remco Diab

Sanofi, Rotkreuz, Risch-Rotkreuz, Switzerland.

Mengjie Yao

Sanofi, Bridgewater, New Jersey, United States.

Imene Gouia

Sanofi, Health Economics and Value Assessment, Gentilly, France.

Michelle Lee

Sanofi, Bridgewater, New Jersey, United States.

Ahmed Abd Almalik Daak

Sanofi, Cambridge, Massachusetts, United States.