Publication | Closed Access
Classification of Epigenetic Biomarkers with Atomically Thin Nanopores
18
Citations
24
References
2018
Year
EngineeringMatched FilterBiochemical SensorsMolecular BiologyBiomedical EngineeringElectronic PropertiesEpigeneticsDna NanotechnologyBiosensing SystemsBioimagingNanosensorMolecular DiagnosticsSignal Processing ArchitecturesMolecular ImagingBiophysicsWearable BiosensorsBiomedical AnalysisBioinformaticsBiomolecular ScienceSingle-molecule DetectionChromatinBiomedical SensorsBiomedical DiagnosticsBioelectronicsEpigenomicsLab-on-a-chipMolecular BiophysicsMedicineNanoporesEpigenetic Biomarkers
We use the electronic properties of 2D solid-state nanopore materials to propose a versatile and generally applicable biosensor technology by using a combination of molecular dynamics, nanoscale device simulations, and statistical signal processing algorithms. As a case study, we explore the classification of three epigenetic biomarkers, the methyl-CpG binding domain 1 (MBD-1), MeCP2, and γ-cyclodextrin, attached to double-stranded DNA to identify regions of hyper- or hypomethylations by utilizing a matched filter. We assess the sensing ability of the nanopore device to identify the biomarkers based on their characteristic electronic current signatures. Such a matched filter-based classifier enables real-time identification of the biomarkers that can be easily implemented on chip. This integration of a sensor with signal processing architectures could pave the way toward the development of a multipurpose technology for early disease detection.
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