C Soussain1, S Choquet2, M Blonski3, D Leclercq4, C Houillier5, K Rezai6, F Bijou7, R Houot8, E Boyle9, R Gressin10, E Nicolas-Virelizier11, M Barrie12, C Moluçon-Chabrot13, M L Lelez14, A Clavert15, S Coisy16, S Leruez16, V Touitou17, N Cassoux18, M Daniau19, M Ertault de la Bretonnière20, A El Yamani21, H Ghesquières22, K Hoang-Xuan5. 1. Hematology, Institut Curie, Site Saint-Cloud, France. Electronic address: carole.soussain@curie.fr. 2. Hematology, APHP, Groupe Hospitalier Pitié-Salpêtrière, Paris, France. 3. Neurology, Centre Hospitalier Universitaire de Nancy, France. 4. Neuro-Radiology, APHP, Groupe Hospitalier Pitié-Salpêtrière, Paris, France. 5. APHP, Sorbonne Université, IHU, ICM, Neurology,Groupe Hospitalier Pitié-Salpêtrière, Paris, France. 6. Radio-Pharmacology, Institut Curie, Site Saint-Cloud, France. 7. Hematology, Institut Bergonié, Bordeaux, France. 8. Univ. Rennes, CHU Rennes, Department of Hematology, Inserm, MICMAC (MIcroenvironment, Cell differentiation, iMmunology and Cancer), UMR_S 1236, F-35000, Rennes, France. 9. Hematology, Centre Hospitalier Universitaire de Lille, France. 10. Hematology, Centre Hospitalier Universitaire de Grenoble, France. 11. Hematology, Centre Léon Berard, Lyon, France. 12. Neuro-Oncology, Centre Hospitalier Universitaire la Timone, Marseille, France. 13. Hematology, Centre Hospitalier Universitaire de Clermont-Ferrand, France. 14. Ophthalmology, Centre Hospitalier Universitaire, Tours, France. 15. Hematology, Centre Hospitalier Universitaire d'Angers, France. 16. Ophthalmology, Centre Hospitalier Universitaire d'Angers, France. 17. Ophthalmology, APHP, Groupe Hospitalier Pitié-Salpêtrière, Paris, France. 18. Ophthalmology, Institut Curie, Site Paris, Université Paris V Descartes et PSL (Paris Science et Lettre), Paris, France. 19. Molecular biology, Institut du cerveau et de la moëlle, Groupe Hospitalier Pitié-Salpêtrière, Paris, France. 20. Hematology and cell Therapy, Centre hospitalier universitaire, Université de Tours. 21. Hematology, Centre Hospitalier de Blois, France. 22. Hematology, Centre Hospitalier Lyon Sud, Université Claude Bernard Lyon 1, Pierre-Bénite, France.
Abstract
BACKGROUND: Primary central nervous system lymphomas (PCNSLs) are mainly diffuse large B-cell lymphomas (DLBCLs) of the non-germinal centre B-cell subtype, with unmet medical needs. This study aimed to evaluate the efficacy and toxicity of ibrutinib in DLBCL-PCNSL PATIENTS AND METHODS: This prospective, multicentre, phase II study involved patients with relapse or refractory(R/R) DLBCL-PCNSL or primary vitreoretinal lymphoma. The treatment consisted of ibrutinib (560 mg/day) until disease progression or unacceptable toxicity occurred. The primary outcome was the disease control (DC) rate after two months of treatment (P0 < 10%; P1 > 30%). RESULTS: Fifty-two patients were recruited. Forty-four patients were evaluable for response. After 2 months of treatment, the DC was 70% in evaluable patients and 62% in the intent-to-treat analysis, including 10 complete responses (19%), 17 partial responses (33%) and 5 stable diseases (10%). With a median follow-up of 25.7 months (range, 0.7-30.5), the median progression-free and overall survivals were 4.8 months (95% confidence interval [CI]; 2.8-12.7) and 19.2 months (95% CI; 7.2-NR), respectively. Thirteen patients received ibrutinib for more than 12 months. Two patients experienced pulmonary aspergillosis with a favourable (n = 1) or fatal outcome (n = 1). Ibrutinib was detectable in the cerebrospinal fluid (CSF). The clinical response to ibrutinib seemed independent of the gene mutations in the BCR pathway. CONCLUSION: Ibrutinib showed clinical activity in the brain, the CSF and the intraocular compartment and was tolerated in R/R PCNSL. The addition of ibrutinib to standard methotrexate-base induction chemotherapy will be further evaluated in the first-line treatment. CLINICAL TRIAL NUMBER: NCT02542514.
BACKGROUND:Primary central nervous system lymphomas (PCNSLs) are mainly diffuse large B-cell lymphomas (DLBCLs) of the non-germinal centre B-cell subtype, with unmet medical needs. This study aimed to evaluate the efficacy and toxicity of ibrutinib in DLBCL-PCNSL PATIENTS AND METHODS: This prospective, multicentre, phase II study involved patients with relapse or refractory(R/R) DLBCL-PCNSL or primary vitreoretinal lymphoma. The treatment consisted of ibrutinib (560 mg/day) until disease progression or unacceptable toxicity occurred. The primary outcome was the disease control (DC) rate after two months of treatment (P0 < 10%; P1 > 30%). RESULTS: Fifty-two patients were recruited. Forty-four patients were evaluable for response. After 2 months of treatment, the DC was 70% in evaluable patients and 62% in the intent-to-treat analysis, including 10 complete responses (19%), 17 partial responses (33%) and 5 stable diseases (10%). With a median follow-up of 25.7 months (range, 0.7-30.5), the median progression-free and overall survivals were 4.8 months (95% confidence interval [CI]; 2.8-12.7) and 19.2 months (95% CI; 7.2-NR), respectively. Thirteen patients received ibrutinib for more than 12 months. Two patients experienced pulmonary aspergillosis with a favourable (n = 1) or fatal outcome (n = 1). Ibrutinib was detectable in the cerebrospinal fluid (CSF). The clinical response to ibrutinib seemed independent of the gene mutations in the BCR pathway. CONCLUSION:Ibrutinib showed clinical activity in the brain, the CSF and the intraocular compartment and was tolerated in R/R PCNSL. The addition of ibrutinib to standard methotrexate-base induction chemotherapy will be further evaluated in the first-line treatment. CLINICAL TRIAL NUMBER: NCT02542514.
Authors: M K Gandhi; T Hoang; S C Law; S Brosda; K O'Rourke; J W D Tobin; F Vari; V Murigneux; L Fink; J Gunawardana; C Gould; H Oey; K Bednarska; S Delecluse; R U Trappe; L Merida de Long; M B Sabdia; G Bhagat; G Hapgood; E Blyth; L Clancy; J Wight; E Hawkes; L M Rimsza; A Maguire; K Bojarczuk; B Chapuy; C Keane Journal: Blood Date: 2021-03-18 Impact factor: 22.113