Correction of transposase sequence bias in ATAC-seq data with rule ensemble modeling

Author:

Wolpe Jacob B1,Martins André L23,Guertin Michael J23ORCID

Affiliation:

1. Department of Biochemistry and Molecular Genetics, University of Virginia , Charlottesville, VA, USA

2. Center for Cell Analysis and Modeling, University of Connecticut , Farmington, CT, USA

3. Department of Genetics and Genome Sciences, University of Connecticut , Farmington, CT, USA

Abstract

Abstract Chromatin accessibility assays have revolutionized the field of transcription regulation by providing single-nucleotide resolution measurements of regulatory features such as promoters and transcription factor binding sites. ATAC-seq directly measures how well the Tn5 transposase accesses chromatinized DNA. Tn5 has a complex sequence bias that is not effectively scaled with traditional bias-correction methods. We model this complex bias using a rule ensemble machine learning approach that integrates information from many input k-mers proximal to the ATAC sequence reads. We effectively characterize and correct single-nucleotide sequence biases and regional sequence biases of the Tn5 enzyme. Correction of enzymatic sequence bias is an important step in interpreting chromatin accessibility assays that aim to infer transcription factor binding and regulatory activity of elements in the genome.

Funder

Bureau of Indian Education

Publisher

Oxford University Press (OUP)

Subject

Applied Mathematics,Computer Science Applications,Genetics,Molecular Biology,Structural Biology

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