Investigation of measurable residual disease in acute myeloid leukemia by DNA methylation patterns

被引:0
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作者
Tanja Božić
Chao-Chung Kuo
Jan Hapala
Julia Franzen
Monika Eipel
Uwe Platzbecker
Martin Kirschner
Fabian Beier
Edgar Jost
Christian Thiede
Wolfgang Wagner
机构
[1] RWTH Aachen University Medical School,Helmholtz
[2] RWTH Aachen University Medical School,Institute for Biomedical Engineering, Stem Cell Biology and Cellular Engineering
[3] Leipzig University Hospital,Institute for Biomedical Engineering – Cell Biology
[4] RWTH Aachen University,Department of Hematology, Cellular Therapy and Hemostaseology
[5] Center for Integrated Oncology Aachen Bonn Cologne Düsseldorf (CIO ABCD),Department of Hematology, Oncology, Hemostaseology and Stem Cell Transplantation, Medical School
[6] University Hospital Carl Gustav Carus,Medical Department I
[7] TU Dresden,undefined
来源
Leukemia | 2022年 / 36卷
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摘要
Assessment of measurable residual disease (MRD) upon treatment of acute myeloid leukemia (AML) remains challenging. It is usually addressed by highly sensitive PCR- or sequencing-based screening of specific mutations, or by multiparametric flow cytometry. However, not all patients have suitable mutations and heterogeneity of surface markers hampers standardization in clinical routine. In this study, we propose an alternative approach to estimate MRD based on AML-associated DNA methylation (DNAm) patterns. We identified four CG dinucleotides (CpGs) that commonly reveal aberrant DNAm in AML and their combination could reliably discern healthy and AML samples. Interestingly, bisulfite amplicon sequencing demonstrated that aberrant DNAm patterns were symmetric on both alleles, indicating that there is epigenetic crosstalk between homologous chromosomes. We trained shallow-learning and deep-learning algorithms to identify anomalous DNAm patterns. The method was then tested on follow-up samples with and without MRD. Notably, even samples that were classified as MRD negative often revealed higher anomaly ratios than healthy controls, which may reflect clonal hematopoiesis. Our results demonstrate that targeted DNAm analysis facilitates reliable discrimination of malignant and healthy samples. However, since healthy samples also comprise few abnormal-classified DNAm reads the approach does not yet reliably discriminate MRD positive and negative samples.
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页码:80 / 89
页数:9
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