asteRIa enables robust interaction modeling between chromatin modifications and epigenetic readers

Author:

Stadler MaraORCID,Lukauskas Saulius,Bartke Till,Müller Christian L.

Abstract

AbstractChromatin, the nucleoprotein complex consisting of DNA and histone proteins, plays a crucial role in regulating gene expression by controlling access to DNA. Chromatin modifications are key players in this regulation, as they help to orchestrate DNA transcription, replication, and repair. These modifications recruit epigenetic “reader” proteins, which mediate downstream events. Most modifications occur in distinctive combinations within a nucleosome, suggesting that epigenetic information can be encoded in combinatorial chromatin modifications. A detailed understanding of how multiple modifications cooperate in recruiting such proteins has, however, remained largely elusive. Here, we integrate nucleosome affinity purification data with high-throughput quantitative proteomics and hierarchical interaction modeling to estimate combinatorial effects of chromatin modifications on protein recruitment. This is facilitated by the computational workflowasteRIawhich combines hierarchical interaction modeling, stability-based model selection, and replicate-consistency checks fora stableestimation ofRobustInteractions among chromatin modifications.asteRIaidentifies several epigenetic reader candidates responding to specificinteractionsbetween chromatin modifications. For the polycomb protein CBX8, we independently validate our results using genome-wide ChIP-Seq and bisulphite datasets. We provide the first quantitative framework for identifying cooperative effects of chromatin modifications on protein binding.

Publisher

Cold Spring Harbor Laboratory

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