Biallelic deletion of 1p32 defines ultra-high-risk myeloma, but monoallelic del(1p32) remains a strong prognostic factor

Anaïs Schavgoulidze(Inserm), Alexis Talbot(Université Paris Cité), Aurore Perrot(Institut universitaire du cancer de Toulouse Oncopole), Titouan Cazaubiel(Université de Bordeaux), Xavier Leleu(Université de Poitiers), Salomon Manier(Lille’s Cardiology Hospital), Laure Buisson(Inserm), Sabrina Mahéo(Inserm), Laura Do Souto Ferreira(Inserm), Luka Pavageau(Inserm), Cyrille Hulin(Université de Bordeaux), Jean‐Pierre Marolleau(Centre Hospitalier Universitaire Amiens-Picardie), Laurent Voillat, Karim Belhadj(Université Paris-Est Créteil), Marion Divoux(Centre Hospitalier Régional et Universitaire de Nancy), Borhane Slama, Sabine Bréchignac(Université Sorbonne Paris Nord), Margaret Macro(Université de Caen Normandie), Anne-Marie Stoppa(Institut Paoli-Calmettes), Laurence Sanhès(Centre Hospitalier de Perpignan), Frédérique Orsini-Piocelle(Centre Hospitalier Annecy Genevois), Jean Fontan(Centre Hospitalier Universitaire de Besançon), Marie‐Lorraine Chrétien(Maison des Sciences sociales et des Humanités de Dijon), Hélène Demarquette, Mohamad Mohty(Sorbonne Université), Hervé Avet‐Loiseau(Inserm), Jill Corre(Inserm)
Blood
November 14, 2022
10.1182/blood.2022017863
Cited by 59Open Access
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Abstract

Cytogenetic abnormalities (CAs) are known to be the preponderant prognostic factor in multiple myeloma. Our team has recently developed a prognostic score based on 6 CAs, with which del(1p32) appears to be the second worst abnormality after del(17p). This study aimed to confirm the adverse effect of 1p32 deletion in patients with newly diagnosed multiple myeloma (NDMM). Among 2551 patients with newly diagnosed multiple myeloma, 11% were harboring del(1p32). Their overall survival (OS) was significantly inferior compared with patients without del(1p32) (median OS: 49 months vs 124 months). Likewise, progression-free survival was significantly shorter. More importantly, biallelic del(1p32) conferred a dramatically poorer prognosis than a monoallelic del(1p32) (median OS: 25 months vs 60 months). As expected, the OS of patients with del(1p32) significantly decreased when this abnormality was associated with other high-risk CAs [del(17p), t(4;14), or gain(1q)]. In the multivariate analysis, del(1p32) appeared as a negative prognostic factor; after adjustment for age and treatment, the risk of progression was 1.3 times higher among patients harboring del(1p32), and the risk of death was 1.9 times higher. At the dawn of risk-adapted treatment strategies, we have confirmed the adverse effect of del(1p32) in multiple myeloma and the relevance of its assessment at diagnosis.

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