Molecular profiling reveals novel gene fusions and genetic markers for refined patient stratification in pediatric acute lymphoblastic leukemia

Risk-adapted treatment protocols conferred remarkable improvement in the survival rates of pediatric acute lymphoblastic leukemia/lymphoma (ALL/LBL). Nevertheless, clinical management is still challenging in certain molecular subgroups and in the presence of alterations associated with an increased...

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Szerzők:	Péterffy Borbála Krizsán Szilvia Egyed Bálint Bedics Gábor Benard-Slagter Anne Palit Sander Erdélyi Dániel Müller Judit Nagy Tibor Hegyi Lajos Bekő Anna Kenéz Lili Anna Jakab Zsuzsanna Péter György Zombori Marianna Csanádi Krisztina Ottóffy Gábor Csernus Katalin Vojcek Ágnes Tiszlavicz Lilla Györgyi Gábor Krisztina Kelemen Ágnes Hauser Péter Kállay Krisztián Kertész Gabriella Gaál Zsuzsanna Szegedi István Barna Gábor Márk Ágnes Haltrich Irén Hevessy Zsuzsanna Ujfalusi Anikó Kajtár Béla Timár Botond Kiss Csongor Kriván Gergely Matolcsy András Savola Suvi Kovács Gábor Bödör Csaba Alpár Donát
Dokumentumtípus:	Cikk
Megjelent:	2025
Sorozat:	MODERN PATHOLOGY 38 No. 6
Tárgyszavak:	Klinikai orvostan
doi:	10.1016/j.modpat.2025.100741
mtmt:	35798493
Online Access:	http://publicatio.bibl.u-szeged.hu/36296


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024	7		\|a 10.1016/j.modpat.2025.100741 \|2 doi
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245	1	0	\|a Molecular profiling reveals novel gene fusions and genetic markers for refined patient stratification in pediatric acute lymphoblastic leukemia \|h [elektronikus dokumentum] / \|c Péterffy Borbála
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490	0		\|a MODERN PATHOLOGY \|v 38 No. 6
520	3		\|a Risk-adapted treatment protocols conferred remarkable improvement in the survival rates of pediatric acute lymphoblastic leukemia/lymphoma (ALL/LBL). Nevertheless, clinical management is still challenging in certain molecular subgroups and in the presence of alterations associated with an increased rate of relapse. In this study, disease-relevant genomic and transcriptomic profiles were established in a prospective, multicenter, real-world cohort involving 192 children diagnosed with ALL/LBL. Gene fusions were detected in 34.9% of B-ALL and 46.4% of T-ALL patients, with novel chimeric genes involving JAK2, KMT2A, PAX5, RUNX1 and NOTCH1, and with KMT2A-rearranged patients displaying the worst 3-year event-free survival (p=0.019). Non-synonymous mutations were uncovered in 74.9% of the analyzed patients, and a pairwise scrutiny of genetic lesions revealed recurrent clonal selection mechanisms commonly converging on the same pathway (e.g. Ras, JAK/STAT and Notch) in individual patients. Investigation of matched diagnostic and relapse samples unraveled complex subclonal variegation, and mutations affecting the NT5C2, TP53, CDKN2A, and PIK3R1 genes, emerging at the time of relapse. TP53 and CREBBP mutations, even as subclonal aberrations, were associated with shorter 3-year event-free survival among all patients with B-ALL (TP53 mutant vs wild-type: p=0.008, CREBBP mutant vs wild-type: p=0.010); and notably, B-ALL patients showing no measurable residual disease on day 33 could be further stratified based on TP53 mutational status (p<0.001). Our in-depth molecular characterization performed across all risk groups identified novel opportunities for molecularly targeted therapy in 55.9% of high-risk and in 31.6% of standard/intermediate-risk patients.
650		4	\|a Klinikai orvostan
700	0	1	\|a Krizsán Szilvia \|e aut
700	0	1	\|a Egyed Bálint \|e aut
700	0	1	\|a Bedics Gábor \|e aut
700	0	2	\|a Benard-Slagter Anne \|e aut
700	0	2	\|a Palit Sander \|e aut
700	0	2	\|a Erdélyi Dániel \|e aut
700	0	2	\|a Müller Judit \|e aut
700	0	2	\|a Nagy Tibor \|e aut
700	0	2	\|a Hegyi Lajos \|e aut
700	0	2	\|a Bekő Anna \|e aut
700	0	2	\|a Kenéz Lili Anna \|e aut
700	0	2	\|a Jakab Zsuzsanna \|e aut
700	0	2	\|a Péter György \|e aut
700	0	2	\|a Zombori Marianna \|e aut
700	0	2	\|a Csanádi Krisztina \|e aut
700	0	2	\|a Ottóffy Gábor \|e aut
700	0	2	\|a Csernus Katalin \|e aut
700	0	2	\|a Vojcek Ágnes \|e aut
700	0	2	\|a Tiszlavicz Lilla Györgyi \|e aut
700	0	2	\|a Gábor Krisztina \|e aut
700	0	2	\|a Kelemen Ágnes \|e aut
700	0	2	\|a Hauser Péter \|e aut
700	0	2	\|a Kállay Krisztián \|e aut
700	0	2	\|a Kertész Gabriella \|e aut
700	0	2	\|a Gaál Zsuzsanna \|e aut
700	0	2	\|a Szegedi István \|e aut
700	0	2	\|a Barna Gábor \|e aut
700	0	2	\|a Márk Ágnes \|e aut
700	0	2	\|a Haltrich Irén \|e aut
700	0	2	\|a Hevessy Zsuzsanna \|e aut
700	0	2	\|a Ujfalusi Anikó \|e aut
700	0	2	\|a Kajtár Béla \|e aut
700	0	2	\|a Timár Botond \|e aut
700	0	2	\|a Kiss Csongor \|e aut
700	0	2	\|a Kriván Gergely \|e aut
700	0	2	\|a Matolcsy András \|e aut
700	0	2	\|a Savola Suvi \|e aut
700	0	2	\|a Kovács Gábor \|e aut
700	0	2	\|a Bödör Csaba \|e aut
700	0	2	\|a Alpár Donát \|e aut
856	4	0	\|u http://publicatio.bibl.u-szeged.hu/36296/1/PIIS0893395225000377.pdf \|z Dokumentum-elérés

Molecular profiling reveals novel gene fusions and genetic markers for refined patient stratification in pediatric acute lymphoblastic leukemia

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