Construction of a new chromosome-scale, long-read reference genome assembly for the Syrian hamster,Mesocricetus auratus

Author:

Harris R Alan1ORCID,Raveendran Muthuswamy1ORCID,Lyfoung Dustin T2ORCID,Sedlazeck Fritz J1ORCID,Mahmoud Medhat1ORCID,Prall Trent M3ORCID,Karl Julie A3ORCID,Doddapaneni Harshavardhan1ORCID,Meng Qingchang1ORCID,Han Yi1ORCID,Muzny Donna1ORCID,Wiseman Roger W23ORCID,O'Connor David H23ORCID,Rogers Jeffrey1ORCID

Affiliation:

1. Human Genome Sequencing Center and Department of Molecular and Human Genetics, Baylor College of Medicine , Houston, TX 77030, USA

2. Wisconsin National Primate Research Center, University of Wisconsin , 1220 Capitol Court, Madison, WI 53711, USA

3. Department of Pathology and Laboratory Medicine, University of Wisconsin , 3170 UW Medical Foundation Centennial Building (MFCB), 1685 Highland Avenue, Madison, WI 53711, USA

Abstract

AbstractBackgroundThe Syrian hamster (Mesocricetus auratus) has been suggested as a useful mammalian model for a variety of diseases and infections, including infection with respiratory viruses such as SARS-CoV-2. The MesAur1.0 genome assembly was generated in 2013 using whole-genome shotgun sequencing with short-read sequence data. Current more advanced sequencing technologies and assembly methods now permit the generation of near-complete genome assemblies with higher quality and greater continuity.FindingsHere, we report an improved assembly of the M. auratus genome (BCM_Maur_2.0) using Oxford Nanopore Technologies long-read sequencing to produce a chromosome-scale assembly. The total length of the new assembly is 2.46 Gb, similar to the 2.50-Gb length of a previous assembly of this genome, MesAur1.0. BCM_Maur_2.0 exhibits significantly improved continuity, with a scaffold N50 that is 6.7 times greater than MesAur1.0. Furthermore, 21,616 protein-coding genes and 10,459 noncoding genes are annotated in BCM_Maur_2.0 compared to 20,495 protein-coding genes and 4,168 noncoding genes in MesAur1.0. This new assembly also improves the unresolved regions as measured by nucleotide ambiguities, where ∼17.11% of bases in MesAur1.0 were unresolved compared to BCM_Maur_2.0, in which the number of unresolved bases is reduced to 3.00%.ConclusionsAccess to a more complete reference genome with improved accuracy and continuity will facilitate more detailed, comprehensive, and meaningful research results for a wide variety of future studies using Syrian hamsters as models.

Funder

National Institutes of Health

Publisher

Oxford University Press (OUP)

Subject

Computer Science Applications,Health Informatics

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