Benchmarking nanopore methylation analysis by comparison to publicly available bisulphite datasets

Genomic DNA can be sequenced on nanopore devices without the need for fragmentation, amplification or strand synthesis, so long-range methylation information is retained in the data.

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The lower bias, higher mapping rates and greater reproducibility of nanopore methylation analysis than seen with bisulphite data, as revealed by benchmarking results
How nanopore sequencing of unamplified genomic DNA from cancer and matched normal samples enables screening for differentially methylated regions across the whole genome

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Benchmarking nanopore methylation analysis by comparison to publicly available bisulphite datasets

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Benchmarking nanopore methylation analysis by comparison to publicly available bisulphite datasets

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