Engineering a mouse-adapted SADS-CoV and establishing a neonatal mouse model to study its infection
Hanyu Zhang, Mengdi Zhang, Jiaru Zhou, Pengfei Li, Ran Jing, Hongmei Zhu, Yifei Lang, Qigai He, Mengjia Zhang, Wentao Li

TL;DR
Researchers created a mouse model for SADS-CoV, a bat-origin coronavirus, to study its infection and test treatments like remdesivir.
Contribution
A novel mouse-adapted SADS-CoV model was developed using a chimeric virus with a murine spike protein.
Findings
The chimeric mSADS-CoV replicated efficiently in murine cells and caused lethal infection in 2-day-old mice.
The model validated remdesivir's efficacy against SADS-CoV, offering a tool for antiviral testing and pathogenesis studies.
Abstract
Swine acute diarrhea syndrome coronavirus (SADS-CoV) is an emerging bat-origin alphacoronavirus causing severe disease in neonatal piglets, with significant economic losses to the swine industry. The virus exhibits a broad species tropism, infecting cells derived from pigs, humans, and mice, highlighting its potential for cross-species transmission. Due to drawbacks associated with the use of young piglets, there is a need for an appropriate small animal model to study SADS-CoV biology. Here we established a mouse infection model based on a murinized mutant of the virus, mSADS-CoV, in which the ectodomain of the viral spike protein was replaced by that of the murine coronavirus mouse hepatitis virus. This chimeric virus, generated through targeted RNA recombination, replicated efficiently in murine cell cultures and exhibited an age-dependent infection in neonatal mice that was lethal…
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Taxonomy
TopicsAnimal Virus Infections Studies · SARS-CoV-2 and COVID-19 Research · Viral gastroenteritis research and epidemiology
