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G+C content dominates intrinsic nucleosome occupancy

Identifieur interne : 002794 ( Main/Exploration ); précédent : 002793; suivant : 002795

G+C content dominates intrinsic nucleosome occupancy

Auteurs : Desiree Tillo [Canada] ; Timothy R. Hughes [Canada]

Source :

RBID : PMC:2808325

Descripteurs français

English descriptors

Abstract

Background

The relative preference of nucleosomes to form on individual DNA sequences plays a major role in genome packaging. A wide variety of DNA sequence features are believed to influence nucleosome formation, including periodic dinucleotide signals, poly-A stretches and other short motifs, and sequence properties that influence DNA structure, including base content. It was recently shown by Kaplan et al. that a probabilistic model using composition of all 5-mers within a nucleosome-sized tiling window accurately predicts intrinsic nucleosome occupancy across an entire genome in vitro. However, the model is complicated, and it is not clear which specific DNA sequence properties are most important for intrinsic nucleosome-forming preferences.

Results

We find that a simple linear combination of only 14 simple DNA sequence attributes (G+C content, two transformations of dinucleotide composition, and the frequency of eleven 4-bp sequences) explains nucleosome occupancy in vitro and in vivo in a manner comparable to the Kaplan model. G+C content and frequency of AAAA are the most important features. G+C content is dominant, alone explaining ~50% of the variation in nucleosome occupancy in vitro.

Conclusions

Our findings provide a dramatically simplified means to predict and understand intrinsic nucleosome occupancy. G+C content may dominate because it both reduces frequency of poly-A-like stretches and correlates with many other DNA structural characteristics. Since G+C content is enriched or depleted at many types of features in diverse eukaryotic genomes, our results suggest that variation in nucleotide composition may have a widespread and direct influence on chromatin structure.


Url:
DOI: 10.1186/1471-2105-10-442
PubMed: 20028554
PubMed Central: 2808325


Affiliations:


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Le document en format XML

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