Human methylome studies SRP576746 Track Settings
 
CD19-CAR T cells undergo exhaustion epigenetic programming in patients with acute lymphoblastic leukemia [CD8+ T Cells]

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 SRX28262777  CpG methylation  CD8+ T Cells / SRX28262777 (CpG methylation)   Schema 
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 SRX28262779  CpG methylation  CD8+ T Cells / SRX28262779 (CpG methylation)   Schema 
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 SRX28262780  CpG methylation  CD8+ T Cells / SRX28262780 (CpG methylation)   Schema 
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 SRX28262781  CpG methylation  CD8+ T Cells / SRX28262781 (CpG methylation)   Schema 
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 SRX28262782  CpG methylation  CD8+ T Cells / SRX28262782 (CpG methylation)   Schema 
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 SRX28262783  CpG methylation  CD8+ T Cells / SRX28262783 (CpG methylation)   Schema 
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 SRX28262784  CpG methylation  CD8+ T Cells / SRX28262784 (CpG methylation)   Schema 
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 SRX28262785  CpG methylation  CD8+ T Cells / SRX28262785 (CpG methylation)   Schema 
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 SRX28262786  CpG methylation  CD8+ T Cells / SRX28262786 (CpG methylation)   Schema 
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 SRX28262787  CpG methylation  CD8+ T Cells / SRX28262787 (CpG methylation)   Schema 
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 SRX28262788  CpG methylation  CD8+ T Cells / SRX28262788 (CpG methylation)   Schema 
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 SRX28262789  CpG methylation  CD8+ T Cells / SRX28262789 (CpG methylation)   Schema 
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 SRX28262790  CpG methylation  CD8+ T Cells / SRX28262790 (CpG methylation)   Schema 
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 SRX28262791  CpG methylation  CD8+ T Cells / SRX28262791 (CpG methylation)   Schema 
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 SRX28262792  CpG methylation  CD8+ T Cells / SRX28262792 (CpG methylation)   Schema 
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 SRX28262794  CpG methylation  CD8+ T Cells / SRX28262794 (CpG methylation)   Schema 
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 SRX28262796  CpG methylation  CD8+ T Cells / SRX28262796 (CpG methylation)   Schema 
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 SRX28262797  CpG methylation  CD8+ T Cells / SRX28262797 (CpG methylation)   Schema 
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 SRX28262798  CpG methylation  CD8+ T Cells / SRX28262798 (CpG methylation)   Schema 
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 SRX28262799  CpG methylation  CD8+ T Cells / SRX28262799 (CpG methylation)   Schema 
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 SRX28262800  CpG methylation  CD8+ T Cells / SRX28262800 (CpG methylation)   Schema 
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 SRX28262800  HMR  CD8+ T Cells / SRX28262800 (HMR)   Schema 
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 SRX28262801  CpG methylation  CD8+ T Cells / SRX28262801 (CpG methylation)   Schema 
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 SRX28262802  CpG methylation  CD8+ T Cells / SRX28262802 (CpG methylation)   Schema 
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 SRX28262803  CpG methylation  CD8+ T Cells / SRX28262803 (CpG methylation)   Schema 
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 SRX28262804  CpG methylation  CD8+ T Cells / SRX28262804 (CpG methylation)   Schema 
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 SRX28262805  CpG methylation  CD8+ T Cells / SRX28262805 (CpG methylation)   Schema 
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 SRX28262806  CpG methylation  CD8+ T Cells / SRX28262806 (CpG methylation)   Schema 
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 SRX28262806  HMR  CD8+ T Cells / SRX28262806 (HMR)   Schema 
    

Study title: CD19-CAR T cells undergo exhaustion epigenetic programming in patients with acute lymphoblastic leukemia
SRA: SRP576746
GEO: not found
Pubmed: not found

Experiment Label Methylation Coverage HMRs HMR size AMRs AMR size PMDs PMD size Conversion Details
SRX28262777 CD8+ T Cells 0.741 22.1 56169 956.3 1457 1045.9 3118 10481.2 0.991 title: GSM5677818 Pre-infusion - rep1, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Before Week 0", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262778 CD8+ T Cells 0.786 23.1 64126 999.3 1439 1031.8 4201 13347.6 0.993 title: GSM5677819 Pre-infusion - rep2, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Before Week 0", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262779 CD8+ T Cells 0.800 11.0 49685 1041.8 406 961.4 2265 18352.9 0.989 title: GSM5677820 Pre-infusion - rep3, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Before Week 0", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262780 CD8+ T Cells 0.802 16.7 60209 978.4 702 919.1 4307 12319.0 0.978 title: GSM5677821 Pre-infusion - rep4, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Before Week 0", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262781 CD8+ T Cells 0.812 8.4 43318 1194.2 455 909.5 1542 17490.8 0.923 title: GSM5677822 GMP - rep1, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 0", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262782 CD8+ T Cells 0.753 22.9 55528 955.3 1039 1093.4 2722 9335.9 0.984 title: GSM5677823 GMP - rep2, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 0", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262783 CD8+ T Cells 0.767 43.2 62598 972.0 1347 1084.3 3550 10841.7 0.993 title: GSM5677824 GMP - rep3, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 0", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262784 CD8+ T Cells 0.748 20.3 59242 942.8 1158 1108.3 3376 9509.5 0.981 title: GSM5677825 GMP - rep4, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 0", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262785 CD8+ T Cells 0.718 22.6 58522 918.2 1156 1091.9 3540 10203.4 0.992 title: GSM5677826 GMP - rep5, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 0", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262786 CD8+ T Cells 0.735 19.4 58181 925.4 678 945.5 3882 8715.6 0.991 title: GSM5677827 GMP - rep6, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 0", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262787 CD8+ T Cells 0.748 10.4 48758 1075.9 703 1035.5 1931 16950.3 0.978 title: GSM5677828 GMP - rep7, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 0", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262788 CD8+ T Cells 0.788 25.0 60874 1008.0 995 1026.9 3595 13312.0 0.979 title: GSM5677829 GMP - rep8, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 0", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262789 CD8+ T Cells 0.785 10.8 42121 1237.7 183 996.3 1535 17899.1 0.975 title: GSM5677830 GMP - rep9, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 0", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262790 CD8+ T Cells 0.804 9.3 44582 1155.7 184 1148.1 1859 17130.1 0.992 title: GSM5677831 GMP - rep10, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 0", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262791 CD8+ T Cells 0.791 17.8 54003 984.5 261 979.2 2774 9788.2 0.987 title: GSM5677832 GMP - rep11, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 0", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262792 CD8+ T Cells 0.724 6.1 34977 1291.7 124 1538.3 934 20858.1 0.978 title: GSM5677833 GMP - rep12, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 0", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262793 CD8+ T Cells 0.730 21.7 58492 919.7 1104 1049.2 3222 10298.1 0.994 title: GSM5677834 GMP - rep13, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 0", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262794 CD8+ T Cells 0.766 16.3 52246 1051.4 535 946.5 2960 11041.6 0.984 title: GSM5677835 Week1 - rep1, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 1", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262795 CD8+ T Cells 0.753 17.2 55841 932.9 630 909.5 3164 10051.6 0.993 title: GSM5677836 Week1 - rep2, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 1", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262796 CD8+ T Cells 0.780 14.9 46996 1264.7 2303 976.0 2661 10881.5 0.945 title: GSM5677838 Week1 - rep4, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 1", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262797 CD8+ T Cells 0.739 19.5 51166 1023.8 782 1068.2 2684 10940.5 0.992 title: GSM5677839 Week2 - rep1, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 2", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262798 CD8+ T Cells 0.683 26.9 51148 1018.7 961 1075.1 2042 10565.6 0.993 title: GSM5677840 Week2 - rep2, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 2", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262799 CD8+ T Cells 0.717 20.6 50568 1064.7 768 1160.0 1561 12820.8 0.988 title: GSM5677841 Week2 - rep3, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 2", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262800 CD8+ T Cells 0.717 19.0 51288 986.5 584 963.7 2572 9316.7 0.992 title: GSM5677842 Week2 - rep4, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 2", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262801 CD8+ T Cells 0.692 15.8 49913 1043.5 900 1055.4 2262 10722.8 0.992 title: GSM5677843 Week2 - rep5, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 2", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262802 CD8+ T Cells 0.749 25.8 49908 1375.2 9295 1105.0 2618 22591.2 0.912 title: GSM5677844 Week3 - rep1, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 3", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262803 CD8+ T Cells 0.690 34.7 56333 952.2 1140 1132.8 2065 12878.4 0.994 title: GSM5677845 Week3 - rep2, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 3", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262804 CD8+ T Cells 0.726 19.5 49283 1225.6 2038 1021.7 2111 16434.0 0.970 title: GSM5677846 Week3 - rep3, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 3", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262805 CD8+ T Cells 0.706 5.3 33139 1467.2 141 1091.9 887 23433.0 0.990 title: GSM5677847 Week4 - rep1, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 4", "geo_loc_name": "missing", "collection_date": "missing"}
SRX28262806 CD8+ T Cells 0.753 31.6 61174 908.9 650 952.3 2788 10678.0 0.992 title: GSM5677837 Week1 - rep3, Homo sapiens, Bisulfite-Seq; {"source_name": "CD19-CAR T cells", "disease": "B-cell acute lymphoblastic leukemia", "cell_type": "CD8+ T cells", "timepoint": "Week 1", "geo_loc_name": "missing", "collection_date": "missing"}

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.