TY - JOUR
T1 - LSC17 score complements genetics and measurable residual disease in acute myeloid leukemia
T2 - an ALFA study
AU - Vasseur, Loïc
AU - Fenwarth, Laurène
AU - Lambert, Jérǒme
AU - de Botton, Stéphane
AU - Figeac, Martin
AU - Villenet, Céline
AU - Heiblig, Maël
AU - Dumas, Pierre Yves
AU - Récher, Christian
AU - Berthon, Céline
AU - Lemasle, Emilie
AU - Lebon, Delphine
AU - Lambert, Juliette
AU - Terré, Christine
AU - Celli-Lebras, Karine
AU - Dombret, Hervé
AU - Preudhomme, Claude
AU - Cheok, Meyling
AU - Itzykson, Raphael
AU - Duployez, Nicolas
N1 - Publisher Copyright:
© 2023 by The American Society of Hematology.
PY - 2023/8/8
Y1 - 2023/8/8
N2 - Whether the LSC17 gene expression can improve risk stratification in the context of next generation sequencing-based risk stratification and measurable residual disease (MRD) in patients with intensively treated AML has not been explored. We analyzed LSC17 in 504 adult patients prospectively treated in the ALFA-0702 trial. RUNX1 or TP53 mutations were associated with higher LSC1 scores while CEBPA and NPM1 mutations were associated with lower scores. Patients with high LSC17 scores had a lower rate of complete response (CR) in a multivariable analysis (odds ratio, 0.41; P = .0007), accounting for European LeukemiaNet 2022 (ELN22), age, and white blood cell count (WBC). LSC17-high status was associated with shorter overall survival (OS) (3-year OS: 70.0% vs 52.7% in patients with LSC17-low status; P < .0001). In a multivariable analysis considering ELN22, age, and WBC, patients with LSC17-high status had shorter disease-free survival (DFS) (hazard ratio [HR], 1.36; P = .048) than those with LSC17-low status. In 123 patients with NPM1-mutated AML in CR, LSC17- high status predicted poorer DFS (HR, 2.34; P = .01), independent of age, WBC, ELN22 risk, and NPM1-MRD. LSC-low status and negative NPM1-MRD identified a subset comprising 48% of patients with mutated NPM1 with a 3-year OS from CR of 93.1% compared with 60.7% in those with LSC17-high status and/or positive NPM1-MRD (P = .0001). Overall, LSC17 assessment refines genetic risk stratification in adult patients with AML treated intensively. Combined with MRD, LSC17 identifies a subset of patients with NPM1-mutated AML with excellent clinical outcome.
AB - Whether the LSC17 gene expression can improve risk stratification in the context of next generation sequencing-based risk stratification and measurable residual disease (MRD) in patients with intensively treated AML has not been explored. We analyzed LSC17 in 504 adult patients prospectively treated in the ALFA-0702 trial. RUNX1 or TP53 mutations were associated with higher LSC1 scores while CEBPA and NPM1 mutations were associated with lower scores. Patients with high LSC17 scores had a lower rate of complete response (CR) in a multivariable analysis (odds ratio, 0.41; P = .0007), accounting for European LeukemiaNet 2022 (ELN22), age, and white blood cell count (WBC). LSC17-high status was associated with shorter overall survival (OS) (3-year OS: 70.0% vs 52.7% in patients with LSC17-low status; P < .0001). In a multivariable analysis considering ELN22, age, and WBC, patients with LSC17-high status had shorter disease-free survival (DFS) (hazard ratio [HR], 1.36; P = .048) than those with LSC17-low status. In 123 patients with NPM1-mutated AML in CR, LSC17- high status predicted poorer DFS (HR, 2.34; P = .01), independent of age, WBC, ELN22 risk, and NPM1-MRD. LSC-low status and negative NPM1-MRD identified a subset comprising 48% of patients with mutated NPM1 with a 3-year OS from CR of 93.1% compared with 60.7% in those with LSC17-high status and/or positive NPM1-MRD (P = .0001). Overall, LSC17 assessment refines genetic risk stratification in adult patients with AML treated intensively. Combined with MRD, LSC17 identifies a subset of patients with NPM1-mutated AML with excellent clinical outcome.
UR - http://www.scopus.com/inward/record.url?scp=85164914562&partnerID=8YFLogxK
U2 - 10.1182/bloodadvances.2023010155
DO - 10.1182/bloodadvances.2023010155
M3 - Article
C2 - 37205853
AN - SCOPUS:85164914562
SN - 2473-9529
VL - 7
SP - 4024
EP - 4034
JO - Blood Advances
JF - Blood Advances
IS - 15
ER -