A DNA methylation atlas of normal human cell types

被引:0
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作者
Netanel Loyfer
Judith Magenheim
Ayelet Peretz
Gordon Cann
Joerg Bredno
Agnes Klochendler
Ilana Fox-Fisher
Sapir Shabi-Porat
Merav Hecht
Tsuria Pelet
Joshua Moss
Zeina Drawshy
Hamed Amini
Patriss Moradi
Sudharani Nagaraju
Dvora Bauman
David Shveiky
Shay Porat
Uri Dior
Gurion Rivkin
Omer Or
Nir Hirshoren
Einat Carmon
Alon Pikarsky
Abed Khalaileh
Gideon Zamir
Ronit Grinbaum
Machmud Abu Gazala
Ido Mizrahi
Noam Shussman
Amit Korach
Ori Wald
Uzi Izhar
Eldad Erez
Vladimir Yutkin
Yaacov Samet
Devorah Rotnemer Golinkin
Kirsty L. Spalding
Henrik Druid
Peter Arner
A. M. James Shapiro
Markus Grompe
Alex Aravanis
Oliver Venn
Arash Jamshidi
Ruth Shemer
Yuval Dor
Benjamin Glaser
Tommy Kaplan
机构
[1] The Hebrew University of Jerusalem,School of Computer Science and Engineering
[2] Hebrew University of Jerusalem,Department of Developmental Biology and Cancer Research, Institute for Medical Research Israel
[3] GRAIL,Canada, Hadassah Medical Center and Faculty of Medicine
[4] Inc.,Sharett Institute of Oncology
[5] Hadassah Hebrew University Medical Center,Department of Obstetrics and Gynecology, Hadassah Medical Center and Faculty of Medicine
[6] Hebrew University of Jerusalem,Department of Orthopedics, Hadassah Medical Center and Faculty of Medicine
[7] Hebrew University of Jerusalem,Department of Otolaryngology, Hadassah Medical Center and Faculty of Medicine
[8] Hebrew University of Jerusalem,Department of General Surgery, Hadassah Medical Center and Faculty of Medicine
[9] Hebrew University of Jerusalem,Surgery Division, Hadassah Medical Center and Faculty of Medicine
[10] Hebrew University of Jerusalem,Department of Cardiothoracic Surgery, Hadassah Medical Center and Faculty of Medicine
[11] Hebrew University of Jerusalem,Department of Urology, Hadassah Medical Center and Faculty of Medicine
[12] Hebrew University of Jerusalem,Department of Vascular Surgery
[13] Shaare Zedek Medical Center,Department of Endocrinology and Metabolism, Hadassah Medical Center and Faculty of Medicine
[14] Hebrew University of Jerusalem,Department of Cell and Molecular Biology
[15] Karolinska Institutet,Department of Oncology
[16] Karolinska Institutet,Pathology
[17] The National Board of Forensic Medicine,Department of Forensic Medicine
[18] Department of Medicine (H7) and Karolinska University Hospital,Department of Surgery and the Clinical Islet Transplant Program
[19] Karolinska Institutet,Department of Surgery
[20] University of Alberta,undefined
[21] Papé Family Pediatric Research Institute,undefined
[22] Oregon Health & Science University,undefined
[23] Samson Assuta Ashdod University Hospital,undefined
[24] Illumina,undefined
[25] Inc.,undefined
来源
Nature | 2023年 / 613卷
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摘要
DNA methylation is a fundamental epigenetic mark that governs gene expression and chromatin organization, thus providing a window into cellular identity and developmental processes1. Current datasets typically include only a fraction of methylation sites and are often based either on cell lines that underwent massive changes in culture or on tissues containing unspecified mixtures of cells2–5. Here we describe a human methylome atlas, based on deep whole-genome bisulfite sequencing, allowing fragment-level analysis across thousands of unique markers for 39 cell types sorted from 205 healthy tissue samples. Replicates of the same cell type are more than 99.5% identical, demonstrating the robustness of cell identity programmes to environmental perturbation. Unsupervised clustering of the atlas recapitulates key elements of tissue ontogeny and identifies methylation patterns retained since embryonic development. Loci uniquely unmethylated in an individual cell type often reside in transcriptional enhancers and contain DNA binding sites for tissue-specific transcriptional regulators. Uniquely hypermethylated loci are rare and are enriched for CpG islands, Polycomb targets and CTCF binding sites, suggesting a new role in shaping cell-type-specific chromatin looping. The atlas provides an essential resource for study of gene regulation and disease-associated genetic variants, and a wealth of potential tissue-specific biomarkers for use in liquid biopsies.
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页码:355 / 364
页数:9
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