Abstract

Genomes assembled de novo from short reads are highly fragmented relative to the finished chromosomes of Homo sapiens and key model organisms generated by the Human Genome Project. To address this problem, we need scalable, cost-effective methods to obtain assemblies with chromosome-scale contiguity. Here we show that genome-wide chromatin interaction data sets, such as those generated by Hi-C, are a rich source of long-range information for assigning, ordering and orienting genomic sequences to chromosomes, including across centromeres. To exploit this finding, we developed an algorithm that uses Hi-C data for ultra-long-range scaffolding of de novo genome assemblies. We demonstrate the approach by combining shotgun fragment and short jump mate-pair sequences with Hi-C data to generate chromosome-scale de novo assemblies of the human, mouse and Drosophila genomes, achieving--for the human genome--98% accuracy in assigning scaffolds to chromosome groups and 99% accuracy in ordering and orienting scaffolds within chromosome groups. Hi-C data can also be used to validate chromosomal translocations in cancer genomes.

Keywords

GenomeChromatinChromosome conformation captureBiologyComputational biologyChromosomeHuman genomeGeneticsHomo sapiensGenomicsGene

MeSH Terms

AlgorithmsAnimalsBase SequenceChromatinChromosome MappingContig MappingDrosophilaHumansMiceMolecular Sequence DataSequence AnalysisDNA

Affiliated Institutions

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Publication Info

Year
2013
Type
article
Volume
31
Issue
12
Pages
1119-1125
Citations
1548
Access
Closed

Social Impact

Social media, news, blog, policy document mentions

Citation Metrics

1548
OpenAlex
103
Influential
1369
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Cite This

Joshua N. Burton, Andrew Adey, Rupali P Patwardhan et al. (2013). Chromosome-scale scaffolding of de novo genome assemblies based on chromatin interactions. Nature Biotechnology , 31 (12) , 1119-1125. https://doi.org/10.1038/nbt.2727

Identifiers

DOI
10.1038/nbt.2727
PMID
24185095
PMCID
PMC4117202

Data Quality

Data completeness: 90%