Genomic-transcriptomic analysis identifies the Syrian hamster as a superior animal model for human diseases

Chuchu Wang
Zhenguo Cheng
Jinxin Miao
Xia Xue
Yunshu Dong
Li Zhao
Haoran Guo
Jianyao Wang
Zhizhong Wang
Shuangshuang Lu
Guangming Fang
Ying Peng
Yafei Zhai
Zhongxian Zhang
Dongling Gao
Zhimin Wang
Pengju Wang
Lirong Zhang
Louisa S Chard Dunmall
Jun Wang
Wenxue Tang
Xiaowei Li
Zhongren Ding
Xiaoyan Zhao
Ling Li
Nicholas R. Lemoine
Zhongde Wang
Daniel Tonge
Wenjie Tan
Jianzeng Dong
Yaohe Wang

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Abstract

Background

The Syrian hamster ( Mesocricetus auratus ) has shown promise as a human diseases model, recapitulating features of different human diseases including COVID-19. However, the landscape of its genome and transcriptome has not been systematically dissected, restricting its potential applications.

Results

Here we provide a complete analysis of the genome and transcriptome of the Syrian hamster and found that its lineage diverged from that of the Chinese hamster ( Cricetulus griseus ) around 29.4 million years ago. 21,387 protein-coding genes were identified, with 90.03% of the 2.56G base pair sequence being anchored to 22 chromosomes. Further comparison of the transcriptomes from 15 tissues of the Syrian hamster revealed that the Syrian hamster shares a pattern of alternative splicing modes more similar to humans, compared to rats and mice. An integrated genomic-transcriptomic analysis revealed that the Syrian hamster also has genetic and biological advantages as a superior animal model for cardiovascular diseases. Strikingly, several genes involved in SARS-COV-2 infection, including ACE2, present a higher homology with humans compared to other rodents and show the same function as their human counterparts.

Conclusion

The detailed molecular characterisation of the Syrian hamster in the present study opens a wealth of fundamental resources from this small rodent for future research into human disease pathology and treatment.

Version published to 10.1186/s12864-025-11393-4
Mar 24, 2025
Version published to 10.21203/rs.3.rs-3962413/v1 on Research Square
Mar 12, 2024

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