Modeling gene expression using chromatin features in various cellular contexts

BACKGROUND: Previous work has demonstrated that chromatin feature levels correlate with gene expression. The ENCODE project enables us to further explore this relationship using an unprecedented volume of data. Expression levels from more than 100,000 promoters were measured using a variety of high-...

Full description

Saved in:
Bibliographic Details
Published inGenome biology Vol. 13; no. 9; p. R53
Main Authors Dong, Xianjun, Greven, Melissa C, Kundaje, Anshul, Djebali, Sarah, Brown, James B, Cheng, Chao, Gingeras, Tom R, Gerstein, Mark, Guigó, Roderic, Birney, Ewan, Weng, Zhiping
Format Journal Article
LanguageEnglish
Published England Springer-Verlag 05.09.2012
BioMed Central
Subjects
chromatin
Chromatin - chemistry
Chromatin - metabolism
Cromatina
deoxyribonuclease I
gene expression
Genoma humà
Genome, Human
Genètica
histones
Histones - genetics
Histones - metabolism
human cell lines
Humans
Models estadístics
Models, Genetic
Models, Statistical
Organ Specificity
Poly A - metabolism
RNA
RNA, Messenger - chemistry
RNA, Messenger - metabolism
transcription (genetics)
Transcription, Genetic
Online AccessGet full text

Cover

More Information
Summary:BACKGROUND: Previous work has demonstrated that chromatin feature levels correlate with gene expression. The ENCODE project enables us to further explore this relationship using an unprecedented volume of data. Expression levels from more than 100,000 promoters were measured using a variety of high-throughput techniques applied to RNA extracted by different protocols from different cellular compartments of several human cell lines. ENCODE also generated the genome-wide mapping of eleven histone marks, one histone variant, and DNase I hypersensitivity sites in seven cell lines. RESULTS: We built a novel quantitative model to study the relationship between chromatin features and expression levels. Our study not only confirms that the general relationships found in previous studies hold across various cell lines, but also makes new suggestions about the relationship between chromatin features and gene expression levels. We found that expression status and expression levels can be predicted by different groups of chromatin features, both with high accuracy. We also found that expression levels measured by CAGE are better predicted than by RNA-PET or RNA-Seq, and different categories of chromatin features are the most predictive of expression for different RNA measurement methods. Additionally, PolyA+ RNA is overall more predictable than PolyA- RNA among different cell compartments, and PolyA+ cytosolic RNA measured with RNA-Seq is more predictable than PolyA+ nuclear RNA, while the opposite is true for PolyA- RNA. CONCLUSIONS: Our study provides new insights into transcriptional regulation by analyzing chromatin features in different cellular contexts.
Bibliography:http://dx.doi.org/10.1186/gb-2012-13-9-r53
ObjectType-Article-1
SourceType-Scholarly Journals-1
ObjectType-Feature-2
content type line 23
ISSN:1465-6906
1474-760X
1465-6914
1474-760X
DOI:10.1186/gb-2012-13-9-r53