Mouse methylome studies SRP349681 Track Settings
 
The distinct effects of MEK and GSK3 inhibition upon the DNA methylome and transcriptome of mouse embryonic stem cells [Embryonic Stem Cells]

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 SRX13343934  HMR  Embryonic Stem Cells / SRX13343934 (HMR)   Data format 
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 SRX13343934  CpG methylation  Embryonic Stem Cells / SRX13343934 (CpG methylation)   Data format 
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 SRX13343935  HMR  Embryonic Stem Cells / SRX13343935 (HMR)   Data format 
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 SRX13343935  CpG methylation  Embryonic Stem Cells / SRX13343935 (CpG methylation)   Data format 
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 SRX13343936  CpG methylation  Embryonic Stem Cells / SRX13343936 (CpG methylation)   Data format 
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 SRX13343937  CpG methylation  Embryonic Stem Cells / SRX13343937 (CpG methylation)   Data format 
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 SRX13343938  HMR  Embryonic Stem Cells / SRX13343938 (HMR)   Data format 
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 SRX13343938  CpG methylation  Embryonic Stem Cells / SRX13343938 (CpG methylation)   Data format 
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 SRX13343939  HMR  Embryonic Stem Cells / SRX13343939 (HMR)   Data format 
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 SRX13343939  CpG methylation  Embryonic Stem Cells / SRX13343939 (CpG methylation)   Data format 
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 SRX13343940  HMR  Embryonic Stem Cells / SRX13343940 (HMR)   Data format 
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 SRX13343940  CpG methylation  Embryonic Stem Cells / SRX13343940 (CpG methylation)   Data format 
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 SRX13343941  CpG methylation  Embryonic Stem Cells / SRX13343941 (CpG methylation)   Data format 
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 SRX13343942  HMR  Embryonic Stem Cells / SRX13343942 (HMR)   Data format 
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 SRX13343942  CpG methylation  Embryonic Stem Cells / SRX13343942 (CpG methylation)   Data format 
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 SRX13343943  CpG methylation  Embryonic Stem Cells / SRX13343943 (CpG methylation)   Data format 
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 SRX13343944  CpG methylation  Embryonic Stem Cells / SRX13343944 (CpG methylation)   Data format 
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 SRX13343945  CpG methylation  Embryonic Stem Cells / SRX13343945 (CpG methylation)   Data format 
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 SRX13343946  CpG methylation  Embryonic Stem Cells / SRX13343946 (CpG methylation)   Data format 
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 SRX13343947  CpG methylation  Embryonic Stem Cells / SRX13343947 (CpG methylation)   Data format 
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 SRX13343948  CpG methylation  Embryonic Stem Cells / SRX13343948 (CpG methylation)   Data format 
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 SRX13343949  HMR  Embryonic Stem Cells / SRX13343949 (HMR)   Data format 
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 SRX13343949  CpG methylation  Embryonic Stem Cells / SRX13343949 (CpG methylation)   Data format 
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 SRX13343950  CpG methylation  Embryonic Stem Cells / SRX13343950 (CpG methylation)   Data format 
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 SRX13343951  CpG methylation  Embryonic Stem Cells / SRX13343951 (CpG methylation)   Data format 
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 SRX13343952  CpG methylation  Embryonic Stem Cells / SRX13343952 (CpG methylation)   Data format 
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 SRX13343953  CpG methylation  Embryonic Stem Cells / SRX13343953 (CpG methylation)   Data format 
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 SRX13343954  CpG methylation  Embryonic Stem Cells / SRX13343954 (CpG methylation)   Data format 
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 SRX13343955  CpG methylation  Embryonic Stem Cells / SRX13343955 (CpG methylation)   Data format 
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 SRX13343956  CpG methylation  Embryonic Stem Cells / SRX13343956 (CpG methylation)   Data format 
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 SRX13343957  CpG methylation  Embryonic Stem Cells / SRX13343957 (CpG methylation)   Data format 
    
Assembly: Mouse Jun. 2020 (GRCm39/mm39)

Study title: The distinct effects of MEK and GSK3 inhibition upon the DNA methylome and transcriptome of mouse embryonic stem cells
SRA: SRP349681
GEO: GSE190402
Pubmed: not found

Experiment Label Methylation Coverage HMRs HMR size AMRs AMR size PMDs PMD size Conversion Title
SRX13343934 Embryonic Stem Cells 0.616 3.1 31810 2589.4 3 961.3 688 75527.7 0.995 GSM5723130: 24d_GSK3i_L_2_WGBS; Mus musculus; Bisulfite-Seq
SRX13343935 Embryonic Stem Cells 0.675 2.4 32274 2515.6 4 1123.5 987 99698.9 0.994 GSM5723131: 24d_GSK3i_L_3_WGBS; Mus musculus; Bisulfite-Seq
SRX13343936 Embryonic Stem Cells 0.414 3.0 6921 14641.8 4 1031.0 766 318554.2 0.996 GSM5723148: 8d_2i_L_2_WGBS; Mus musculus; Bisulfite-Seq
SRX13343937 Embryonic Stem Cells 0.428 4.0 22923 6303.8 7 1256.0 1248 178333.9 0.996 GSM5723149: 8d_2i_L_3_WGBS; Mus musculus; Bisulfite-Seq
SRX13343938 Embryonic Stem Cells 0.661 3.8 40413 2188.5 5 796.0 1425 72090.6 0.994 GSM5723150: 8d_GSK3i_L_2_WGBS; Mus musculus; Bisulfite-Seq
SRX13343939 Embryonic Stem Cells 0.638 3.8 38070 2158.9 12 1218.5 1305 63705.0 0.995 GSM5723151: 8d_GSK3i_L_3_WGBS; Mus musculus; Bisulfite-Seq
SRX13343940 Embryonic Stem Cells 0.706 2.1 29300 2170.2 4 807.8 692 123745.2 0.991 GSM5723152: 8d_S_L_2_WGBS; Mus musculus; Bisulfite-Seq
SRX13343941 Embryonic Stem Cells 0.719 2.0 27085 2120.7 2 668.5 618 120053.3 0.991 GSM5723153: 8d_S_L_3_WGBS; Mus musculus; Bisulfite-Seq
SRX13343942 Embryonic Stem Cells 0.623 3.3 29927 2266.3 4 761.0 760 56155.3 0.994 GSM5723132: 2d_1uM_MEKi_L_2_WGBS; Mus musculus; Bisulfite-Seq
SRX13343943 Embryonic Stem Cells 0.631 2.2 26546 2778.2 2 885.0 635 116480.8 0.994 GSM5723133: 2d_1uM_MEKi_L_3_WGBS; Mus musculus; Bisulfite-Seq
SRX13343944 Embryonic Stem Cells 0.559 2.3 24503 4058.2 0 0.0 703 158075.2 0.995 GSM5723134: 4d_1uM_MEKi_L_2_WGBS; Mus musculus; Bisulfite-Seq
SRX13343945 Embryonic Stem Cells 0.565 2.2 25248 4041.7 0 0.0 572 185559.1 0.995 GSM5723135: 4d_1uM_MEKi_L_3_WGBS; Mus musculus; Bisulfite-Seq
SRX13343946 Embryonic Stem Cells 0.488 2.3 22271 5237.3 2 965.5 710 231886.8 0.995 GSM5723136: 6d_1uM_MEKi_L_2_WGBS; Mus musculus; Bisulfite-Seq
SRX13343947 Embryonic Stem Cells 0.490 2.6 23751 5341.6 0 0.0 822 209029.8 0.995 GSM5723137: 6d_1uM_MEKi_L_3_WGBS; Mus musculus; Bisulfite-Seq
SRX13343948 Embryonic Stem Cells 0.624 2.1 25551 3365.9 1 656.0 565 196588.5 0.991 GSM5723138: 8d_0.2uM_MEKi_L_2_WGBS; Mus musculus; Bisulfite-Seq
SRX13343949 Embryonic Stem Cells 0.643 2.3 26095 2910.6 4 828.5 871 125555.1 0.991 GSM5723139: 8d_0.2uM_MEKi_L_3_WGBS; Mus musculus; Bisulfite-Seq
SRX13343950 Embryonic Stem Cells 0.524 2.2 25687 4351.0 0 0.0 664 215181.9 0.993 GSM5723140: 8d_0.4uM_MEKi_L_2_WGBS; Mus musculus; Bisulfite-Seq
SRX13343951 Embryonic Stem Cells 0.551 2.0 25258 4245.7 1 815.0 631 225242.5 0.994 GSM5723141: 8d_0.4uM_MEKi_L_3_WGBS; Mus musculus; Bisulfite-Seq
SRX13343952 Embryonic Stem Cells 0.450 1.6 1 483565.0 1 750.0 557 455605.4 0.995 GSM5723142: 8d_0.6uM_MEKi_L_2_WGBS; Mus musculus; Bisulfite-Seq
SRX13343953 Embryonic Stem Cells 0.437 2.7 7652 14572.6 0 0.0 753 290430.5 0.995 GSM5723143: 8d_0.6uM_MEKi_L_3_WGBS; Mus musculus; Bisulfite-Seq
SRX13343954 Embryonic Stem Cells 0.389 2.3 3 882394.0 0 0.0 6 10533590.7 0.995 GSM5723144: 8d_0.8uM_MEKi_L_2_WGBS; Mus musculus; Bisulfite-Seq
SRX13343955 Embryonic Stem Cells 0.393 3.1 25 141429.0 2 722.0 26 6740997.9 0.995 GSM5723145: 8d_0.8uM_MEKi_L_3_WGBS; Mus musculus; Bisulfite-Seq
SRX13343956 Embryonic Stem Cells 0.392 3.1 14 172680.3 2 686.0 32 6439010.3 0.995 GSM5723146: 8d_1uM_MEKi_L_2_WGBS; Mus musculus; Bisulfite-Seq
SRX13343957 Embryonic Stem Cells 0.423 3.6 18171 8163.8 2 720.5 938 214856.6 0.995 GSM5723147: 8d_1uM_MEKi_L_3_WGBS; Mus musculus; Bisulfite-Seq

Methods

All analysis was done using a bisulfite sequnecing data analysis pipeline DNMTools developed in the Smith lab at USC.

Mapping reads from bisulfite sequencing: Bisulfite treated reads are mapped to the genomes with the abismal program. Input reads are filtered by their quality, and adapter sequences in the 3' end of reads are trimmed. This is done with cutadapt. Uniquely mapped reads with mismatches/indels below given threshold are retained. For pair-end reads, if the two mates overlap, the overlapping part of the mate with lower quality is discarded. After mapping, we use the format command in dnmtools to merge mates for paired-end reads. We use the dnmtools uniq command to randomly select one from multiple reads mapped exactly to the same location. Without random oligos as UMIs, this is our best indication of PCR duplicates.

Estimating methylation levels: After reads are mapped and filtered, the dnmtools counts command is used to obtain read coverage and estimate methylation levels at individual cytosine sites. We count the number of methylated reads (those containing a C) and the number of unmethylated reads (those containing a T) at each nucleotide in a mapped read that corresponds to a cytosine in the reference genome. The methylation level of that cytosine is estimated as the ratio of methylated to total reads covering that cytosine. For cytosines in the symmetric CpG sequence context, reads from the both strands are collapsed to give a single estimate. Very rarely do the levels differ between strands (typically only if there has been a substitution, as in a somatic mutation), and this approach gives a better estimate.

Bisulfite conversion rate: The bisulfite conversion rate for an experiment is estimated with the dnmtools bsrate command, which computes the fraction of successfully converted nucleotides in reads (those read out as Ts) among all nucleotides in the reads mapped that map over cytosines in the reference genome. This is done either using a spike-in (e.g., lambda), the mitochondrial DNA, or the nuclear genome. In the latter case, only non-CpG sites are used. While this latter approach can be impacted by non-CpG cytosine methylation, in practice it never amounts to much.

Identifying hypomethylated regions (HMRs): In most mammalian cells, the majority of the genome has high methylation, and regions of low methylation are typically the interesting features. (This seems to be true for essentially all healthy differentiated cell types, but not cells of very early embryogenesis, various germ cells and precursors, and placental lineage cells.) These are valleys of low methylation are called hypomethylated regions (HMR) for historical reasons. To identify the HMRs, we use the dnmtools hmr command, which uses a statistical model that accounts for both the methylation level fluctations and the varying amounts of data available at each CpG site.

Partially methylated domains: Partially methylated domains are large genomic regions showing partial methylation observed in immortalized cell lines and cancerous cells. The pmd program is used to identify PMDs.

Allele-specific methylation: Allele-Specific methylated regions refers to regions where the parental allele is differentially methylated compared to the maternal allele. The program allelic is used to compute allele-specific methylation score can be computed for each CpG site by testing the linkage between methylation status of adjacent reads, and the program amrfinder is used to identify regions with allele-specific methylation.

For more detailed description of the methods of each step, please refer to the DNMTools documentation.