Publication date: Oct 12, 2024
Coronaviruses (CoVs) represent a serious threat to human health and have become a major transmissible, endemic, and causative pathogen in humans; they represent a major health concern, given their ability to cause infectious diseases. Bats are natural hosts for diverse viruses. Many transmission events of CoVs and identification of multiple novel CoVs in bats has increased attention towards their capacity to serve as hosts for zoonotic viruses. In this study, 61 bats from Yunnan Province were analyzed, identifying seven CoVs, including three α- and two β-CoVs with full-genome sequences. Among the five identified alpha-CoVs, four belong to the Decacovirus subgenus and one to the Minunacovirus subgenus. Two beta-CoVs were also identified, both belonging to the Sarbecovirus subgenus. The genetic structures revealed similarities to known strains such as HKU10 and SARS-CoV-2, along with novel findings such as the Minunacovirus subgenus CoV YJ3c/f and unique ORF patterns. Our results demonstrated that strain JCC9 has a unique recombination pattern and shows a higher binding affinity to civet and pangolin ACE2 receptors, then the HpJC8xc strain transmits and recombines between hosts (bats), indicating a potential risk of crossing the interspecies barrier and infecting other animals. The CoVs detected in the bats studied in this research exhibit high diversity. Genomic analysis revealed that CoVs in bats undergo frequent recombination events. Furthermore, recombination patterns and evolutionary analyses suggest that alpha-CoVs are more prone to cross-species transmission across different bat families/genera, whereas beta-CoVs demonstrate host specificity and tend to co-evolve with their bat hosts. Our finding suggest that bats, as hosts of CoVs, be constantly monitored to prevent outbreaks of new infections caused by viruses passing across interspecies barriers, and consequently, viral diseases in humans or livestock.
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Semantics
Type | Source | Name |
---|---|---|
disease | IDO | pathogen |
disease | MESH | infectious diseases |
disease | IDO | host |
disease | MESH | infections |
disease | MESH | viral diseases |
pathway | REACTOME | Reproduction |
drug | DRUGBANK | Coenzyme M |
disease | MESH | COVID 19 |
drug | DRUGBANK | Nonoxynol-9 |
disease | MESH | emerging infectious diseases |
drug | DRUGBANK | Ademetionine |
disease | IDO | infection |
disease | IDO | protein |
drug | DRUGBANK | Esomeprazole |
drug | DRUGBANK | Fenamole |
drug | DRUGBANK | Pentaerythritol tetranitrate |
disease | MESH | zoonotic spillover |
drug | DRUGBANK | Prazosin |
disease | MESH | Coronavirus infections |
disease | IDO | infectivity |
disease | IDO | cell |