doi: 10.1126/science.1162253.
Epub 2008 Dec 4.
Divergent transcription from active promoters
Affiliations
- PMID: 19056940
- PMCID: PMC2692996
- DOI: 10.1126/science.1162253
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Divergent transcription from active promoters
Science.
.
Abstract
Transcription initiation by RNA polymerase II (RNAPII) is thought to occur unidirectionally from most genes. Here, we present evidence of widespread divergent transcription at protein-encoding gene promoters. Transcription start site-associated RNAs (TSSa-RNAs) nonrandomly flank active promoters, with peaks of antisense and sense short RNAs at 250 nucleotides upstream and 50 nucleotides downstream of TSSs, respectively. Northern analysis shows that TSSa-RNAs are subsets of an RNA population 20 to 90 nucleotides in length. Promoter-associated RNAPII and H3K4-trimethylated histones, transcription initiation hallmarks, colocalize at sense and antisense TSSa-RNA positions; however, H3K79-dimethylated histones, characteristic of elongating RNAPII, are only present downstream of TSSs. These results suggest that divergent transcription over short distances is common for active promoters and may help promoter regions maintain a state poised for subsequent regulation.
Figures
The distribution of TSSa-RNAs around TSSs shows divergent transcription. (A) Histogram of the distance from each TSSa-RNA to all associated gene TSSs (4). Counts of TSSa-RNA 5′ positions relative to gene TSSs are binned in 20 nucleotide windows. Red and blue bars represent bins of TSSa-RNAs in the sense and anti-sense orientation with respect to gene transcription, respectively. (B) Percentage of annotated mouse genes with indicated number of associating TSSa-RNAs.
In ES cells, TSSa-RNA associated genes are primarily expressed. (A) ES cell expression data was separated into 4 bins based on Log2 signal intensity levels; off = 1-4, low = 5-8, med = 6-12, and high ≥ 13 (9). Gene counts for each gene expression level bin are shown. (B) The ratio of sense to anti-sense reads in each expression bin.
Transcripts from TSSa-RNA associated regions are primarily 20-90 nts long. (A) Map of the sense TSSa-RNA Rnf12 region. (B) Northern analysis for the Rnf12 sense TSSa-RNA using probe 1 in A. Lane 1 is a 10 bp ladder. Lanes 2-5 are detection controls with 15, and 1.5, 0.75, and 0 fMol of synthetic RNAs (RNA oligo 1a/b in A). Lanes 6-8 are material recovered from the enrichment procedure using DNA oligo 1 in A. Lane 6 is J1 ES cell enriched material (ESC), lane 7 is Hela enriched material (H-), and lane 8 is Hela + 15 fMol synthetic RNA oligos 1a/b in A enriched material (H+). (C) Map of the anti-sense TSSa-RNA Ccdc52 region. (D) Northern analysis for the Ccdc52 anti-sense TSSa-RNA using probe 1 in A. Lanes 1-4 are as lanes 2-5 in B, except using RNA oligo 2 in C. Lanes 5-7 are material recovered from the enrichment procedure using DNA oligo 2. Lane 5 is J1 ES cell enriched material (ESC), lane 6 is Hela enriched material (H-), and lane 7 is Hela + 15 fMol synthetic TSSa-RNA-2 in C enriched material (H+). Bracket marks ESC specific transcripts; * marks background band.
Relationship between TSSa-RNAs and chromatin structure. (A) Percentage of genes associated with indicated chromatin marks. T-test gives p-values < 2.2e-16 for all marks. (B) Schematic of factor binding site mapping using forward and reverse Chip-seq reads. The midpoint between the forward and reverse reads defines the bound factor location. (C) Chromosomal position vs. enrichment ratio for H3K4me3-modified nucleosomes and RNAPII for a representative gene Mknk2. (D) Metagene profiles for forward (green) and reverse (yellow) reads for ChIP-seq data (first three panels) and TSSa-RNAs from the sense (red) and anti-sense (blue) strand (bottom panel). Panels are aligned at the TSS. The TSS is denoted by the arrow. Black numbers on the profiles define the midpoint between forward and reverse peaks. Red and blue bars above the ChIP-seq profiles represent sense and anti-sense TSSa-RNA peak maxima.
Comment in
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Transcription. Gene expression--where to start?Science. 2008 Dec 19;322(5909):1804-5. doi: 10.1126/science.1168805. Science. 2008. PMID: 19095933 Free PMC article. No abstract available.
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