High-quality genome (re)assembly using chromosomal contact data

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作者
Hervé Marie-Nelly
Martial Marbouty
Axel Cournac
Jean-François Flot
Gianni Liti
Dante Poggi Parodi
Sylvie Syan
Nancy Guillén
Antoine Margeot
Christophe Zimmer
Romain Koszul
机构
[1] Institut Pasteur,Department of Genomes and Genetics
[2] Groupe Régulation Spatiale des Génomes,undefined
[3] CNRS,undefined
[4] UMR 3525,undefined
[5] Institut Pasteur,undefined
[6] Unité Imagerie et Modélisation,undefined
[7] CNRS,undefined
[8] URA 2582,undefined
[9] Sorbonne Universités,undefined
[10] UPMC Univ Paris06,undefined
[11] IFD,undefined
[12] Max Planck Institute for Dynamics and Self-Organization,undefined
[13] Group Biological Physics and Evolutionary Dynamics,undefined
[14] Institute for Research on Cancer and Ageing of Nice (IRCAN),undefined
[15] CNRS UMR 7284—INSERM U108,undefined
[16] Université de Nice Sophia Antipolis,undefined
[17] IFP Energies Nouvelles,undefined
[18] Institut Pasteur,undefined
[19] Unité Cell Biology of Parasitism,undefined
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摘要
Closing gaps in draft genome assemblies can be costly and time-consuming, and published genomes are therefore often left ‘unfinished.’ Here we show that genome-wide chromosome conformation capture (3C) data can be used to overcome these limitations, and present a computational approach rooted in polymer physics that determines the most likely genome structure using chromosomal contact data. This algorithm—named GRAAL—generates high-quality assemblies of genomes in which repeated and duplicated regions are accurately represented and offers a direct probabilistic interpretation of the computed structures. We first validated GRAAL on the reference genome of Saccharomyces cerevisiae, as well as other yeast isolates, where GRAAL recovered both known and unknown complex chromosomal structural variations. We then applied GRAAL to the finishing of the assembly of Trichoderma reesei and obtained a number of contigs congruent with the know karyotype of this species. Finally, we showed that GRAAL can accurately reconstruct human chromosomes from either fragments generated in silico or contigs obtained from de novo assembly. In all these applications, GRAAL compared favourably to recently published programmes implementing related approaches.
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