Refining risk prediction in pediatric acute lymphoblastic leukemia through DNA methylation profiling

被引:0
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作者
Adrián Mosquera Orgueira
Olga Krali
Carlos Pérez Míguez
Andrés Peleteiro Raíndo
José Ángel Díaz Arias
Marta Sonia González Pérez
Manuel Mateo Pérez Encinas
Manuel Fernández Sanmartín
Daniel Sinnet
Mats Heyman
Gudmar Lönnerholm
Ulrika Norén-Nyström
Kjeld Schmiegelow
Jessica Nordlund
机构
[1] University Hospital of Santiago de Compostela,Department of Hematology
[2] Health Research Institute of Santiago de Compostela,Department of Medical Sciences, Molecular Precision Medicine
[3] Uppsala University,Science for Life Laboratory
[4] Uppsala University,Department of Pediatric Medicine
[5] University Hospital of Santiago de Compostela,Research Center
[6] CHU Sainte-Justine,Department of Pediatrics
[7] Université de Montréal,Childhood Cancer Research Unit
[8] Karolinska Institutet,Department of Women’s and Children’s Health
[9] Astrid Lindgren Children’s Hospital,Department of Clinical Sciences, Pediatrics
[10] Karolinska University Hospital,Pediatrics and Adolescent Medicine, Rigshospitalet, and the Medical Faculty, Institute of Clinical Medicine
[11] Uppsala University,undefined
[12] Umeå University,undefined
[13] University of Copenhagen,undefined
[14] For the Nordic Society of Pediatric Hematology and Oncology (NOPHO),undefined
来源
Clinical Epigenetics | / 16卷
关键词
Pediatric acute lymphoblastic leukemia; Epigenetics; DNA methylation; Machine learning; Artificial intelligence; Relapse risk; Mortality risk; Precision medicine;
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摘要
Acute lymphoblastic leukemia (ALL) is the most prevalent cancer in children, and despite considerable progress in treatment outcomes, relapses still pose significant risks of mortality and long-term complications. To address this challenge, we employed a supervised machine learning technique, specifically random survival forests, to predict the risk of relapse and mortality using array-based DNA methylation data from a cohort of 763 pediatric ALL patients treated in Nordic countries. The relapse risk predictor (RRP) was constructed based on 16 CpG sites, demonstrating c-indexes of 0.667 and 0.677 in the training and test sets, respectively. The mortality risk predictor (MRP), comprising 53 CpG sites, exhibited c-indexes of 0.751 and 0.754 in the training and test sets, respectively. To validate the prognostic value of the predictors, we further analyzed two independent cohorts of Canadian (n = 42) and Nordic (n = 384) ALL patients. The external validation confirmed our findings, with the RRP achieving a c-index of 0.667 in the Canadian cohort, and the RRP and MRP achieving c-indexes of 0.529 and 0.621, respectively, in an independent Nordic cohort. The precision of the RRP and MRP models improved when incorporating traditional risk group data, underscoring the potential for synergistic integration of clinical prognostic factors. The MRP model also enabled the definition of a risk group with high rates of relapse and mortality. Our results demonstrate the potential of DNA methylation as a prognostic factor and a tool to refine risk stratification in pediatric ALL. This may lead to personalized treatment strategies based on epigenetic profiling.
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