J 2025

ATM aberrations in chronic lymphocytic leukemia: del(11q) rather than ATM mutations is an adverse-prognostic biomarker

THORVALDSDOTTIR, Birna; Larry MANSOURI; Lesley-Ann SUTTON; Ferran NADEU; Manja MEGGENDORFER et. al.

Basic information

Original name

ATM aberrations in chronic lymphocytic leukemia: del(11q) rather than ATM mutations is an adverse-prognostic biomarker

Authors

THORVALDSDOTTIR, Birna; Larry MANSOURI; Lesley-Ann SUTTON; Ferran NADEU; Manja MEGGENDORFER; Helen PARKER; Christian BRIEGHEL; Stamatia LAIDOU; Riccardo MOIA; Davide ROSSI; Jana KOTAŠKOVÁ; Julio DELGADO; Ana E RODRIGUEZ-VICENTE; Rocio BENITO; Gian Matteo RIGOLIN; Silvia BONFIGLIO; Lydia SCARFO; Mattias MATTSSON; Zadie DAVIS; Panagiotis BALIAKAS; Inmaculada RAPADO; Fatima MIRAS; Joaquin MARTINEZ-LOPEZ; de la Serna JAVIER; Hernandez Rivas Jesus MARIA; Maria Jose LARRAYOZ; Maria Jose CALASANZ; Karin E SMEDBY; Blanca ESPINET; Anna PUIGGROS; Lars BULLINGER; Francesc BOSCH; Barbara TAZON-VEGA; Fanny BARAN-MARSZAK; David OSCIER; Florence NGUYEN-KHAC; Thorsten ZENZ; Maria Jose TEROL; Antonio CUNEO; Maria HERNANDEZ-SANCHEZ; Šárka POSPÍŠILOVÁ; Gianluca GAIDANO; Carsten U NIEMANN; Elias CAMPO; Jonathan C STREFFORD; Paolo GHIA; Kostas STAMATOPOULOS and Richard ROSENQUIST

Edition

Leukemia, London, Nature Publishing Group, 2025, 0887-6924

Other information

Language

English

Type of outcome

Article in a journal

Country of publisher

United Kingdom of Great Britain and Northern Ireland

Confidentiality degree

is not subject to a state or trade secret

References:

URL

Organization

Lékařská fakulta – Repository – Repository

DOI

https://doi.org/10.1038/s41375-025-02615-5

UT WoS

001473957800001

EID Scopus

2-s2.0-105003449208

Links

LX22NPO5102, research and development project. NU21-08-00237, research and development project.
Changed: 26/9/2025 00:50, RNDr. Daniel Jakubík

Abstract

In the original language

lt;1% of M-CLL cases. While univariable analysis revealed shorter TTFT for Binet A patients with any ATM aberration compared to ATM-wildtype, multivariable analysis identified only del(11q), trisomy 12, SF3B1, and EGR2 mutations as independent prognosticators of shorter TTFT among Binet A patients and within M-CLL and U-CLL subgroups. These findings highlight del(11q), and not ATM mutations, as a key biomarker of increased risk of early progression and need for therapy, particularly in otherwise indolent M-CLL, providing insights into risk-stratification and therapeutic decision-making.
Displayed: 16/12/2025 22:18