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Molecular profiling of immunoglobulin heavy-chain gene rearrangements unveils new potential prognostic markers for multiple myeloma patients

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Autor/a

Medina, Alejandro

Jiménez, Cristina

Sarasquete, M. Eugenia

González, Marcos

Chillón, M. Carmen

Balanzategui, Ana

Prieto-Conde, Isabel

García-Álvarez, María

Puig, Noemí

González-Calle, Verónica

Alcoceba, Miguel

Cuenca, Isabel

Barrio, Santiago

Escalante, Fernando

Gutierrez, Norma

Gironella, Mercedes

Hernández, Miguel T.

Sureda, Anna

Oriol, Albert

Bladé Creixenti, Juan

Lahuerta, J. J

San Miguel, Jesus F.

Mateos, M. V

Martínez-López, Joaquín

Calasanz, M.J

García-Sanz, Ramón

Universitat Autònoma de Barcelona

Fecha de publicación

2020

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Resumen

Altres ajuts: This work was partially supported by[...] , CIBERONC-CB16/12/00233, and "Una manera de hacer Europa" (Innocampus; CEI-2010-1-0010)". M.G.-A., I.P.-C., and C.J. are supported by the Fundación Española de Hematología y Hemoterapia (FEHH, co-funded by Fundación Cris in the latter case), A.M. by the European Social Fund and the Spanish Education Council through the University of Salamanca, [...]. All Spanish funding is co-sponsored by the European Union FEDER program.

Multiple myeloma is a heterogeneous disease whose pathogenesis has not been completely elucidated. Although B-cell receptors play a crucial role in myeloma pathogenesis, the impact of clonal immunoglobulin heavy-chain features in the outcome has not been extensively explored. Here we present the characterization of complete heavy-chain gene rearrangements in 413 myeloma patients treated in Spanish trials, including 113 patients characterized by next-generation sequencing. Compared to the normal B-cell repertoire, gene selection was biased in myeloma, with significant overrepresentation of IGHV3, IGHD2 and IGHD3, as well as IGHJ4 gene groups. Hypermutation was high in our patients (median: 8.8%). Interestingly, regarding patients who are not candidates for transplantation, a high hypermutation rate (≥7%) and the use of IGHD2 and IGHD3 groups were associated with improved prognostic features and longer survival rates in the univariate analyses. Multivariate analysis revealed prolonged progression-free survival rates for patients using IGHD2/IGHD3 groups (HR: 0.552, 95% CI: 0.361-0.845, p = 0.006), as well as prolonged overall survival rates for patients with hypermutation ≥7% (HR: 0.291, 95% CI: 0.137-0.618, p = 0.001). Our results provide new insights into the molecular characterization of multiple myeloma, highlighting the need to evaluate some of these clonal rearrangement characteristics as new potential prognostic markers.

Tipo de documento

Article

Lengua

Inglés

Materias y palabras clave

Genetics research; Myeloma

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open access

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Articles escrits per personal UAB o publicats per la universitat [88071]