Abstract
Open or accessible chromatin typifies euchromatic regions and helps define cell type-specific transcription programs. DNA replication massively disorders chromatin composition and structure, and how accessible regions are affected by and recover from this disruption has been unclear. Here, we present repli-ATAC-seq, a protocol to profile accessible chromatin genome-wide on replicated DNA starting from 100,000 cells. In this method, replicated DNA is labeled with a short 5-ethynyl-2′-deoxyuridine (EdU) pulse in cultured cells and isolated from a population of tagmented fragments for amplification and next-generation sequencing. Repli-ATAC-seq provides high-resolution information on chromatin dynamics after DNA replication and reveals new insights into the interplay between DNA replication, transcription, and the chromatin landscape.
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Stewart-Morgan, K. R., & Groth, A. (2023). Profiling Chromatin Accessibility on Replicated DNA with repli-ATAC-Seq. In Methods in Molecular Biology (Vol. 2611, pp. 71–84). Humana Press Inc. https://doi.org/10.1007/978-1-0716-2899-7_6
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