Epigenetic features support the diagnosis of B-cell prolymphocytic leukemia and identify 2 clinicobiological subtypes

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Grant support

This work was partially developed at the Centro Esther Koplowitz (Barcelona, Spain). This research was funded by the Accelerator award Cancer Research UK/Italian Association for Cancer Research/Spanish Association Against Cancer joint funder partnership (J.I.M.-S.), Generalitat de Catalunya Suport Grups de Recerca AGAUR (2021-SGR-1343 [J.I.M.-S.], 2021-SGR-01172 [E.C.], and 2021-SGR-01293 [S.B.]), la Caixa Foundation (CLLEvolution, LCF/PR/HR17/52150017 [HR17-00221LCF] and CLLSYSTEMS- LCF/PR/HR22/52420015 [HR22-00172] Health Research 2017 and 2022 Programs, [E.C.]), Force Hemato (grant reference: 03-2022), French Innovative Leukemia Organization group, Association des Cytogeneticiens de Langue Francaise (grant 2022) and SIRIC-CURAMUS (Cancer United research Associating Medecine, University and Society; grant reference: INCa-DGOS-INSERM_12560, INCa-DGOS-INSERM-ITMO Cancer_18010, and INCa-DGOS-INSERM-ITMO Cancer_18002). M.D.-F. is supported by a postdoctoral grant from the Spanish Association Against Cancer. J.C.S. was supported by research grants from the Kay Kendall Leukemia Fund, and Cancer Research UK (Early Cancer Research Initiative Network on MBL-M3 Accelerator award C42023/A29370).

Análisis de autorías institucional

Charalampopoulou, StellaAutor o CoautorNadeu, FerranAutor o CoautorBea, SilviaAutor o CoautorMartinez-Farran, AresAutor o CoautorAymerich, MartaAutor o CoautorRozman, MariaAutor o CoautorCampo, EliasAutor o CoautorDuran-Ferrer, MartiAutor o CoautorMartin-Subero, Jose IAutor (correspondencia)

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Artículo

Publicado en:Blood Advances. 8 (24): 6297-6307 - 2024-12-24 8(24), DOI: 10.1182/bloodadvances.2024013327

Autores: Charalampopoulou, Stella; Chapiro, Elise; Nadeu, Ferran; Zenz, Thorsten; Bea, Silvia; Martinez-Farran, Ares; Aymerich, Marta; Rozman, Maria; Roos-Weil, Damien; Bernard, Olivier; Susin, Santos A; Parker, Helen; Walewska, Renata; Oakes, Christopher C; Strefford, Jonathan C; Campo, Elias; Matutes, Estela; Duran-Ferrer, Marti; Nguyen-Khac, Florence; Martin-Subero, Jose I

Afiliaciones

Ctr Invest Biomed Red Canc, Madrid, Spain - Autor o Coautor

Gustave Roussy, INSERN, U1170, Villejuif, France - Autor o Coautor

Hosp Clin Barcelona, Pathol Dept, Hematopathol Sect, Barcelona, Spain - Autor o Coautor

Inst Catalana Recerca Estudis & Avancats, Barcelona, Spain - Autor o Coautor

Inst Invest Biomed August Pi & Sunyer, Rossello 149-153, Barcelona 08036, Spain - Autor o Coautor

Ohio State Univ, Div Hematol, Columbus, OH USA - Autor o Coautor

Sorbonne Univ, Hop Pitie Salpetriere, Assistance Publ Hop Paris, Serv dematol Biol, Paris, France - Autor o Coautor

Univ Barcelona, Dept Fonaments Clin, Fac Med, Barcelona, Spain - Autor o Coautor

Univ Hosp Dorset NHS Fdn Trust, Dept Cardiol, Bournemouth, England - Autor o Coautor

Univ Hosp, Dept Med Oncol & Hematol, Zurich, Switzerland - Autor o Coautor

Univ Paris Cite, Sorbonne Univ, Drug Resistance Hematol Malignancies Team, Ctr Rech Cordeliers,INSERM,UMRS 1138, Paris, France - Autor o Coautor

Univ Southampton, Fac Med, Sch Canc Sci, Southampton, England - Autor o Coautor

Univ Zurich, Zurich, Switzerland - Autor o Coautor

Resumen

The recognition of B-cell prolymphocytic leukemia (B-PLL) as a separate entity is controversial based on the current classification systems. Here, we analyzed the DNA methylome of a cohort of 20 B-PLL cases diagnosed according to the guidelines of the International Consensus Classification/Fourth revised edition of the World Health Organization Classification, and compared them with chronic lymphocytic leukemia (CLL), mantle cell lymphoma (MCL), splenic marginal zone lymphoma (SMZL), and normal B-cell subpopulations. Unsupervised principal component analyses suggest that B-PLL is epigenetically distinct from CLL, MCL, and SMZL, which is further supported by robust differential methylation signatures in B-PLL. We also observe that B-PLL can be segregated into 2 epitypes with differential clinicobiological characteristics. B-PLL epitype 1 carries lower immunoglobulin heavy variable somatic hypermutation and a less profound germinal center-related DNA methylation imprint than epitype 2. Furthermore, epitype 1 is significantly enriched in mutations affecting MYC and SF3B1, and displays DNA hypomethylation and gene upregulation signatures enriched in MYC targets. Despite the low sample size, patients from epitype 1 have an inferior overall survival than those of epitype 2. This study provides relevant insights into the biology and differential diagnosis of B-PLL, and potentially identifies 2 subgroups with distinct biological and clinical features.

Palabras clave

AgedDna methylationDna methylomeDynamicsEpigenesis, geneticFemaleHumansImpactLeukemia, lymphocytic, chronic, b-cellLeukemia, prolymphocytic, b-cellLymphomaLymphoma, mantle-cellMaleMutationsSf3b

Indicios de calidad

Impacto bibliométrico. Análisis de la aportación y canal de difusión

El trabajo ha sido publicado en la revista Blood Advances debido a la progresión y el buen impacto que ha alcanzado en los últimos años, según la agencia WoS (JCR), se ha convertido en una referencia en su campo. En el año de publicación del trabajo, 2024 aún no existen indicios calculados, pero en 2023, se encontraba en la posición 12/97, consiguiendo con ello situarse como revista Q1 (Primer Cuartil), en la categoría Hematology.

2025-06-21:

Scopus: 1

Impacto y visibilidad social

Análisis de liderazgo de los autores institucionales

Este trabajo se ha realizado con colaboración internacional, concretamente con investigadores de: France; Switzerland; United Kingdom; United States of America.

Existe un liderazgo significativo ya que algunos de los autores pertenecientes a la institución aparecen como primer o último firmante, se puede apreciar en el detalle: Primer Autor (Charalampopoulou, Eleni Styliani) y Último Autor (Martín Subero, José Ignacio).