Telomere-to-telomere assembly of a complete human X chromosome

被引:0
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作者
Karen H. Miga
Sergey Koren
Arang Rhie
Mitchell R. Vollger
Ariel Gershman
Andrey Bzikadze
Shelise Brooks
Edmund Howe
David Porubsky
Glennis A. Logsdon
Valerie A. Schneider
Tamara Potapova
Jonathan Wood
William Chow
Joel Armstrong
Jeanne Fredrickson
Evgenia Pak
Kristof Tigyi
Milinn Kremitzki
Christopher Markovic
Valerie Maduro
Amalia Dutra
Gerard G. Bouffard
Alexander M. Chang
Nancy F. Hansen
Amy B. Wilfert
Françoise Thibaud-Nissen
Anthony D. Schmitt
Jon-Matthew Belton
Siddarth Selvaraj
Megan Y. Dennis
Daniela C. Soto
Ruta Sahasrabudhe
Gulhan Kaya
Josh Quick
Nicholas J. Loman
Nadine Holmes
Matthew Loose
Urvashi Surti
Rosa ana Risques
Tina A. Graves Lindsay
Robert Fulton
Ira Hall
Benedict Paten
Kerstin Howe
Winston Timp
Alice Young
James C. Mullikin
Pavel A. Pevzner
Jennifer L. Gerton
机构
[1] University of California Santa Cruz,UC Santa Cruz Genomics Institute
[2] Computational and Statistical Genomics Branch,Genome Informatics Section
[3] National Human Genome Research Institute,Department of Genome Sciences
[4] National Institutes of Health,Department of Molecular Biology and Genetics, Department of Biomedical Engineering
[5] University of Washington School of Medicine,Graduate Program in Bioinformatics and Systems Biology
[6] Johns Hopkins University,NIH Intramural Sequencing Center, National Human Genome Research Institute
[7] University of California San Diego,National Center for Biotechnology Information, National Library of Medicine
[8] National Institutes of Health,Department of Pathology
[9] Stowers Institute for Medical Research,Cytogenetic and Microscopy Core, National Human Genome Research Institute
[10] National Institutes of Health,Undiagnosed Diseases Program, National Human Genome Research Institute
[11] Wellcome Sanger Institute,Comparative Genomics Analysis Unit, Cancer Genetics and Comparative Genomics Branch
[12] University of Washington,Department of Biochemistry and Molecular Medicine, Genome Center, MIND Institute
[13] National Institutes of Health,DNA Technologies Core, Genome Center
[14] McDonnell Genome Institute at Washington University,Institute of Microbiology and Infection
[15] National Institutes of Health,DeepSeq, School of Life Sciences
[16] National Human Genome Research Institute,Department of Pathology
[17] National Institutes of Health,Department of Computer Science and Engineering
[18] Arima Genomics,Department of Molecular Genetics and Microbiology, Division of Human Genetics
[19] University of California Davis,Howard Hughes Medical Institute
[20] University of California Davis,undefined
[21] University of Birmingham,undefined
[22] University of Nottingham,undefined
[23] University of Pittsburgh,undefined
[24] University of California San Diego,undefined
[25] Duke University Medical Center,undefined
[26] University of Washington,undefined
来源
Nature | 2020年 / 585卷
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摘要
After two decades of improvements, the current human reference genome (GRCh38) is the most accurate and complete vertebrate genome ever produced. However, no single chromosome has been finished end to end, and hundreds of unresolved gaps persist1,2. Here we present a human genome assembly that surpasses the continuity of GRCh382, along with a gapless, telomere-to-telomere assembly of a human chromosome. This was enabled by high-coverage, ultra-long-read nanopore sequencing of the complete hydatidiform mole CHM13 genome, combined with complementary technologies for quality improvement and validation. Focusing our efforts on the human X chromosome3, we reconstructed the centromeric satellite DNA array (approximately 3.1 Mb) and closed the 29 remaining gaps in the current reference, including new sequences from the human pseudoautosomal regions and from cancer-testis ampliconic gene families (CT-X and GAGE). These sequences will be integrated into future human reference genome releases. In addition, the complete chromosome X, combined with the ultra-long nanopore data, allowed us to map methylation patterns across complex tandem repeats and satellite arrays. Our results demonstrate that finishing the entire human genome is now within reach, and the data presented here will facilitate ongoing efforts to complete the other human chromosomes.
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页码:79 / 84
页数:5
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