Low‐burden TP53 mutations represent frequent genetic events in CLL with an increased risk for treatment initiation

Low‐burden TP53 mutations represent frequent genetic events in CLL with an increased risk for treatment initiation

TP53 aberrations predict chemoresistance and represent a contraindication for the use of standard chemoimmunotherapy in chronic lymphocytic leukaemia (CLL). Recent next‐generation sequencing (NGS)‐based studies have identified frequent low‐burden TP53 mutations with variant allele frequencies below...

Teljes leírás

Elmentve itt :
Bibliográfiai részletek
Szerzők: László Tamás
Kotmayer Lili
Fésüs Viktória
Hegyi Lajos
Gróf Stefánia
Nagy Ákos
Kajtár Béla
Balogh Alexandra
Weisinger Júlia
Masszi Tamás
Nagy Zsolt
Farkas Péter
Demeter Judit
Istenes Ildikó
Szász Róbert
Gergely Lajos
Sulák Adrienn
Borbényi Zita
Lévai Dóra
Schneider Tamás
Pettendi Piroska
Bodai Emese
Szerafin László
Rejtő László
Bátai Árpád
Dömötör Mária Á
Sánta Hermina
Plander Márk
Szendrei Tamás
Hamed Aryan
Andrikovics Hajnalka
Egyed Miklós
Masszi András
Alpár Donát
Matolcsy András
Bödör Csaba
Dokumentumtípus: Cikk
Megjelent: 2024
Sorozat:JOURNAL OF PATHOLOGY: CLINICAL RESEARCH 10 No. 1
Tárgyszavak:
Klinikai orvostan
doi:10.1002/cjp2.351

mtmt:34399695
Online Access:http://publicatio.bibl.u-szeged.hu/29794
Leíró adatok
Tartalmi kivonat:TP53 aberrations predict chemoresistance and represent a contraindication for the use of standard chemoimmunotherapy in chronic lymphocytic leukaemia (CLL). Recent next‐generation sequencing (NGS)‐based studies have identified frequent low‐burden TP53 mutations with variant allele frequencies below 10%, but the clinical impact of these low‐burden TP53 mutations is still a matter of debate. In this study, we aimed to scrutinise the subclonal architecture and clinical impact of TP53 mutations using a sensitive, NGS‐based mutation analysis in a ‘real‐world’ cohort of 901 patients with CLL. In total, 225 TP53 mutations were identified in 17.5% (158/901) of the patients; 48% of these alterations represented high‐burden mutations, while 52% were low‐burden TP53 mutations. Low‐burden mutations as sole alterations were identified in 39% (62/158) of all mutated cases with 82% (51/62) of these being represented by a single low‐burden TP53 mutation. Patients harbouring low‐burden TP53 mutations had significantly lower time to first treatment compared to patients with wild‐type TP53 . Our study has expanded the knowledge on the frequency, clonal architecture, and clinical impact of low‐burden TP53 mutations. By demonstrating that patients with sole low‐burden TP53 variants represent more than one‐third of patients with TP53 mutations and have an increased risk for treatment initiation, our findings strengthen the need to redefine the threshold of TP53 variant reporting to below 10% in the routine diagnostic setting.
Terjedelem/Fizikai jellemzők:12
ISSN:2056-4538

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