KMT2D mutations and TP53 disruptions are poor prognostic biomarkers in mantle cell lymphoma receiving high-dose therapy: a FIL study
Simone Ferrero,
Davide Rossi,
Andrea Rinaldi,
Alessio Bruscaggin,
Valeria Spina,
Christian W. Eskelund,
Andrea Evangelista,
Riccardo Moia,
Ivo Kwee,
Christina Dahl,
Alice Di Rocco,
Vittorio Stefoni,
Fary Diop,
Chiara Favini,
Paola Ghione,
Abdurraouf Mokhtar Mahmoud,
Mattia Schipani,
Arne Kolstad,
Daniela Barbero,
Domenico Novero,
Marco Paulli,
Alberto Zamò,
Mats Jerkeman,
Maria Gomes da Silva,
Armando Santoro,
Annalia Molinari,
Andres Ferreri,
Kirsten Grønbæk,
Andrea Piccin,
Sergio Cortelazzo,
Francesco Bertoni,
Marco Ladetto,
Gianluca Gaidano
Affiliations
Simone Ferrero
Department of Molecular Biotechnologies and Health Sciences - Hematology Division, Università di Torino, Torino, Italy;Hematology Division, AOU Città della Salute e della Scienza di Torino, Torino, Italy
Davide Rossi
Hematology, Oncology Institute of Southern Switzerland, Bellinzona, Switzerland;Universita’ della Svizzera italiana, Institute of Oncology Research, Bellinzona, Switzerland
Andrea Rinaldi
Universita’ della Svizzera italiana, Institute of Oncology Research, Bellinzona, Switzerland
Alessio Bruscaggin
Universita’ della Svizzera italiana, Institute of Oncology Research, Bellinzona, Switzerland
Valeria Spina
Universita’ della Svizzera italiana, Institute of Oncology Research, Bellinzona, Switzerland
Christian W. Eskelund
Department of Hematology, Rigshospitalet, Copenhagen, Denmark;Biotech Research and Innovation Centre, Copenhagen, Denmark
Andrea Evangelista
Clinical Epidemiology, Città della Salute e della Scienza and CPO Piemonte, Torino, Italy
Riccardo Moia
Division of Hematology, Department of Translational Medicine, University of Eastern Piedmont, Novara, Italy
Ivo Kwee
Universita’ della Svizzera italiana, Institute of Oncology Research, Bellinzona, Switzerland;Swiss Institute of Bioinformatics (SIB), Lausanne, Switzerland;Dalle Molle Institute for Artificial Intelligence (IDSIA), Manno, Switzerland
Christina Dahl
Danish Cancer Society Research Center, Copenhagen, Denmark
Alice Di Rocco
Department of Cellular Biotechnologies and Hematology, Policlinico Umberto I, "Sapienza" University of Rome, Roma, Italy
Vittorio Stefoni
Institute of Hematology "L. e A. Seràgnoli", University of Bologna, Bologna, Italy
Fary Diop
Division of Hematology, Department of Translational Medicine, University of Eastern Piedmont, Novara, Italy
Chiara Favini
Division of Hematology, Department of Translational Medicine, University of Eastern Piedmont, Novara, Italy
Paola Ghione
Department of Molecular Biotechnologies and Health Sciences - Hematology Division, Università di Torino, Torino, Italy
Abdurraouf Mokhtar Mahmoud
Division of Hematology, Department of Translational Medicine, University of Eastern Piedmont, Novara, Italy
Mattia Schipani
Division of Hematology, Department of Translational Medicine, University of Eastern Piedmont, Novara, Italy
Arne Kolstad
Department of Oncology, Oslo University Hospital, Oslo, Norway
Daniela Barbero
Department of Molecular Biotechnologies and Health Sciences - Hematology Division, Università di Torino, Torino, Italy
Domenico Novero
First Unit of Pathology, AOU Città della Salute e della Scienza di Torino, Torino, Italy
Marco Paulli
Unit of Anatomic Pathology, Department of Molecular Medicine, Fondazione IRCCS Policlinico San Matteo and Università degli Studi di Pavia, Pavia, Italy
Alberto Zamò
Department of Oncology, Università di Torino, Torino, Italy;Department of Diagnostics and Public Health, University of Verona, Verona, Italy
Mats Jerkeman
Department of Oncology, Lund University Hospital, Lund, Sweden
Maria Gomes da Silva
Department of Hematology, Instituto Português de Oncologia de Lisboa, Lisboa, Portugal
Armando Santoro
Humanitas Cancer Center, Humanitas Clinical and Research Center, Rozzano, Italy
Annalia Molinari
Hematology, Ospedale degli Infermi, Rimini, Italy
Andres Ferreri
Lymphoma Unit, Department of Onco-Haematology, IRCCS San Raffaele Scientific Institute, Milano, Italy
Kirsten Grønbæk
Department of Hematology, Rigshospitalet, Copenhagen, Denmark;Biotech Research and Innovation Centre, Copenhagen, Denmark
Andrea Piccin
Department of Hematology, Ospedale Generale, Bolzano, Italy
Sergio Cortelazzo
Oncology Unit, Humanitas/Gavazzeni Clinic, Bergamo, Italy
Francesco Bertoni
Universita’ della Svizzera italiana, Institute of Oncology Research, Bellinzona, Switzerland
Marco Ladetto
SC Ematologia, Azienda Ospedaliera Santi Antonio e Biagio e Cesare Arrigo, Alessandria, Italy
Gianluca Gaidano
Division of Hematology, Department of Translational Medicine, University of Eastern Piedmont, Novara, Italy
In recent years, the outcome of mantle cell lymphoma (MCL) has improved, especially in younger patients, receiving cytarabine-containing chemoimmunotherapy and autologous stem cell transplantation. Nevertheless, a proportion of MCL patients still experience early failure. To identify biomarkers anticipating failure of intensive chemotherapy in MCL, we performed target resequencing and DNA profiling of purified tumor samples collected from patients enrolled in the prospective FIL-MCL0208 phase 3 trial (high-dose chemoimmunotherapy followed by autologous transplantation and randomized lenalidomide maintenance). Mutations of KMT2D and disruption of TP53 by deletion or mutation associated with an increased risk of progression and death, both in univariate and multivariate analysis. By adding KMT2D mutations and TP53 disruption to the MIPI-c backbone, we derived a new prognostic index, the “MIPI-genetic” (“MIPI- g”). The “MIPI-g” improved the model discrimination ability compared to the MIPI-c alone, defining three risk groups: i) low-risk patients (4-year progression free survival and overall survival of 72.0% and 94.5%); ii) inter-mediate-risk patients (4-year progression free survival and overall survival of 42.2% and 65.8%) and iii) high-risk patients (4-year progression free survival and overall survival of 11.5% and 44.9%). Our results: i) confirm that TP53 disruption identifies a high-risk population characterized by poor sensitivity to conventional or intensified chemotherapy; ii) provide the pivotal evidence that patients harboring KMT2D mutations share the same poor outcome as patients harboring TP53 disruption; and iii) allow to develop a tool for the identification of high-risk MCL patients for whom novel therapeutic strategies need to be investigated. (Trial registered at clinicaltrials.gov identifier: NCT02354313).
