János Bolyai Research Scholarship of the Hungarian Academy of Sciences(TKP2021-NVA-15)
Az orvos-, egészségtudományi- és gyógyszerészképzés tudományos műhelyeinek fejlesztése(EFOP-3.6.3-VEKOP-16-2017-00009)
Funder: EFOP-VEKOP
(BO/00125/22)
(ÚNKP-22-3-II-SE-21)
Subjects:
Clinical medicine
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.
