Multiparameter prediction of myeloid neoplasia risk

被引:0
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作者
Muxin Gu
Sruthi Cheloor Kovilakam
William G. Dunn
Ludovica Marando
Clea Barcena
Irina Mohorianu
Alexandra Smith
Siddhartha P. Kar
Margarete A. Fabre
Moritz Gerstung
Catherine A. Cargo
Luca Malcovati
Pedro M. Quiros
George S. Vassiliou
机构
[1] University of Cambridge,Wellcome
[2] University of Cambridge,MRC Cambridge Stem Cell Institute
[3] Universidad de Oviedo,Department of Haematology
[4] Epidemiology and Cancer Statistics Group,Department of Biochemistry and Molecular Biology
[5] University of York,Early Cancer Institute, Department of Oncology
[6] MRC Integrative Epidemiology Unit,Department of Haematology
[7] University of Bristol,Department of Molecular Medicine
[8] Section of Translational Epidemiology,Department of Hematology
[9] Division of Population Health Sciences,Department of Haematology
[10] Bristol,undefined
[11] Medical School,undefined
[12] University of Bristol,undefined
[13] University of Cambridge,undefined
[14] Centre for Genomics Research,undefined
[15] Discovery Sciences,undefined
[16] BioPharmaceuticals R&D,undefined
[17] AstraZeneca,undefined
[18] Division of Artificial Intelligence in Oncology,undefined
[19] DKFZ,undefined
[20] Haematological Malignancy Diagnostic Service,undefined
[21] St James’s Hospital,undefined
[22] Leeds Teaching Hospitals,undefined
[23] University of Pavia,undefined
[24] Fondazione IRCCS Policlinico San Matteo,undefined
[25] Instituto de Investigación Sanitaria del Principado de Asturias,undefined
[26] ISPA,undefined
[27] Cambridge University Hospitals NHS Trust,undefined
来源
Nature Genetics | 2023年 / 55卷
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摘要
The myeloid neoplasms encompass acute myeloid leukemia, myelodysplastic syndromes and myeloproliferative neoplasms. Most cases arise from the shared ancestor of clonal hematopoiesis (CH). Here we analyze data from 454,340 UK Biobank participants, of whom 1,808 developed a myeloid neoplasm 0–15 years after recruitment. We describe the differences in CH mutational landscapes and hematology/biochemistry test parameters among individuals that later develop myeloid neoplasms (pre-MN) versus controls, finding that disease-specific changes are detectable years before diagnosis. By analyzing differences between ‘pre-MN’ and controls, we develop and validate Cox regression models quantifying the risk of progression to each myeloid neoplasm subtype. We construct ‘MN-predict’, a web application that generates time-dependent predictions with the input of basic blood tests and genetic data. Our study demonstrates that many individuals that develop myeloid neoplasms can be identified years in advance and provides a framework for disease-specific prognostication that will be of substantial use to researchers and physicians.
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页码:1523 / 1530
页数:7
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