Genomic screening of 16 UK native bat species through conservationist networks uncovers coronaviruses with zoonotic potential

Tan, Cedric; Trew, Jahcub; Peacock, Thomas P; Mok, Kai Yi; Hart, Charlie; Lau, Kelvin; Ni, D.R.; Orme, David; Ransome, Emma; Pearse, Will; Coleman, Christopher M.; Bailey, Dalan; Thakur, Nazia; Quantrill, Jessica L.; Sukhova, Ksenia; Richard, Damien; Woodward, Guy; Bell, Thomas; Worledge, Lisa; Nunez-Mino, Joe; Tarlinton, Rachael; Apaa, Ternenge; Matthews, Fiona E.; Barclay, Wendy S.; Dorp, Lucy van; Balloux, François; Savolainen, Vincent

doi:10.1101/2023.01.17.524183

Cited by 4 publications

(9 citation statements)

References 112 publications

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“…We used a semi-nested pan-coronavirus PCR assay that targets a highly conserved region of the RNA-dependent RNA polymerase (RdRp) gene 43 . A recent study performed a comparison of pan-coronavirus PCR approaches using a set of novel bat coronaviruses and found that our selected approach outperformed 3/4 comparison approaches 44 . Among tested pooled swabs collected in 2022, we noted a 1% (5/468), 0% (0/146), and 0% (0/31) pan-coronavirus PCR positivity among the residential white-footed mice, forested white-footed mice, and deer, respectively.…”

Section: Resultsmentioning

confidence: 99%

Section: Pan-coronavirus Pcr Testing Followed By Sequencing Revealed ...mentioning

confidence: 99%

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Survey of white-footed mice in Connecticut, USA reveals low SARS-CoV-2 seroprevalence and infection with divergent betacoronaviruses

Earnest,

Hahn,

Feriancek

et al. 2023

Preprint

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Diverse mammalian species display susceptibility to and infection with SARS-CoV-2. Potential SARS-CoV-2 spillback into rodents is understudied despite their host role for numerous zoonoses and human proximity. We assessed exposure and infection among white-footed mice (Peromyscus leucopus) in Connecticut, USA. We observed 1% (6/540) wild-type neutralizing antibody seroprevalence among 2020-2022 residential mice with no cross-neutralization of variants. We detected no SARS-CoV-2 infections via RT-qPCR, but identified non-SARS-CoV-2 betacoronavirus infections via pan-coronavirus PCR among 1% (5/468) of residential mice. Sequencing revealed two divergent betacoronaviruses, preliminarily namedPeromyscus coronavirus-1and-2. Both belong to theBetacoronavirus 1species and are ∼90% identical to the closest known relative,Porcine hemagglutinating encephalomyelitis virus. Low SARS-CoV-2 seroprevalence suggests white-footed mice may not be sufficiently susceptible or exposed to SARS-CoV-2 to present a long-term human health risk. However, the discovery of divergent, non-SARS-CoV-2 betacoronaviruses expands the diversity of known rodent coronaviruses and further investigation is required to understand their transmission extent.

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Section: Resultsmentioning

confidence: 99%

Section: Pan-coronavirus Pcr Testing Followed By Sequencing Revealed ...mentioning

confidence: 99%

Survey of white-footed mice in Connecticut, USA reveals low SARS-CoV-2 seroprevalence and infection with divergent betacoronaviruses

Earnest,

Hahn,

Feriancek

et al. 2023

Preprint

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“…For example, genetic comparison of the S1/S2 region between SARS-CoV-2 and closely related CoVs from European bats revealed that a single nucleotide substitution is sufficient to produce a functional furin cleavage site identical to that of SARS-CoV-2 in two bat CoV variants, an essential molecular determinant of their zoonotic potential (21). However, this substitution alone is not enough to enable furin cleavage in similar bat CoVs, possibly because it is in a short loop that may not be accessible to the protease (64). The Luchacovirus clade is closely related to SADS-CoV and bat CoV HKU2 (Figure 1 and 2), which are also characterized for having a recombinant S gene that is more similar to betacoronaviruses than alphacoronaviruses (65).…”

Section: Discussionmentioning

confidence: 99%

Detection and characterization of novel luchacoviruses, genusAlphacoronavirus, shed in saliva and feces of meso-carnivores in the northeastern United States

Olarte‐Castillo

Plimpton

McQueary

et al. 2023

Preprint

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Small to mid-sized carnivores, known as meso-carnivores, comprise a group of highly diverse mammals, many of which can easily adapt to anthropogenically disturbed environments. Due to commonly inhabiting urban landscapes, high population densities, and wide home ranges, wild meso-carnivores may get exposed to or spread pathogens to other species. To date, several coronaviruses (family Coronaviridae) have been detected and characterized in domesticated and farmed meso-carnivores, but knowledge of the role of meso-carnivores in the epidemiology of coronaviruses (CoVs) remains limited. To increase our understanding of CoVs circulating in wild meso-carnivores, we screened 300 samples, including feces and tissues, from 9 species of free-ranging wild meso-carnivores in the northeastern United States collected between 2016 and 2022. Using a pan-CoV nested PCR approach, we detected CoVs in fecal samples of animals in three species: fisher (Pekania pennanti), bobcat (Lynx rufus) and red fox (Vulpes vulpes). Next generation sequencing revealed that all the detected viruses belonged to the Luchacovirus subgenus within the Alphacoronavirus genus, previously reported only in rodents and lagomorphs (i.e., rabbits and pikas). Genetic comparison of the 3 prime-end of the genome (~12,000 bp) revealed that although the viruses detected group with, and have a genetic organization similar to other luchacoviruses, they are genetically distinct to luchacoviruses from rodents and lagomorphs. Genetic characterization of the spike (S) protein revealed that these luchacoviruses do not have an identifiable S1/S2 cleavage site but do have highly variable structural loops within S1 that comprise protease cleavage motifs or very similar cleavage motifs to those identified in certain pathogenic CoVs. This study highlights the importance of characterizing the S protein from CoVs in various wild animal species to target specific regions for further experimental analysis and epidemiologic monitoring.

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“…The most likely explanation for this pattern is that some viruses are intrinsically more capable of infecting a diverse range of hosts, possibly by exploiting host-cell machinery that are conserved across different hosts. For example, sarbecoviruses (the subgenus comprising SARS-CoV-2) target the ACE2 host-cell receptor, which is conserved across vertebrates 47,48 , and the high structural conservation of the sarbecovirus spike protein 49 , may explain the observation that single mutations can enable sarbecoviruses to expand their host tropism 50 . In other words, multi-host viruses may have evolved to target more conserved host machinery that reduces the mutational barrier for them to productively infect new hosts.…”

Section: Discussionmentioning

confidence: 99%

“…Due to resource and logistical constraints, surveillance studies of novel pathogens in animals often have sparse geographical and/or temporal coverage 14,15 , as they focus on selected host and pathogen taxa. Further, many of these studies do not perform downstream characterisation of the novel viruses recovered, and may lack sensitivity due to the use of PCR pre-screening to prioritise samples for sequencing 16 . As such, our understanding of which viruses can, or are likely to emerge, and in which settings is poor.…”

Section: Introductionmentioning

confidence: 99%

Crossing host boundaries: the evolutionary drivers and correlates of viral host jumps

Tan,

van Dorp,

Balloux

2023

Preprint

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Most emerging and re-emerging infectious diseases stem from viruses that naturally circulate in non-human vertebrates. When these viruses cross over into humans, they can cause disease outbreaks and epidemics. While zoonotic host jumps have been extensively studied from an ecological perspective, little attention has gone into characterising the evolutionary drivers and correlates underlying these events. To address this gap, we harnessed the entirety of publicly available viral genomic data, employing a comprehensive suite of network and phylogenetic analyses. We address a series of questions concerning the evolutionary mechanisms underpinning viral host jumps. Notably, we challenge conventional assumptions about the directionality of host jumps, demonstrating that humans are as much a source as a sink for viral spillover events, insofar we infer more viruses to have jumped from humans to other animals, than from animals to humans. Moreover, we demonstrate heightened evolution in viral lineages that involve putative host jumps. We further observe that the mutational threshold associated with a host jump is lower for viruses with broad host ranges. Finally, we show that the genomic targets of natural selection upon a successful host jump vary across different viral families with either structural or auxiliary genes being the prime targets of selection. Collectively, our results illuminate some of the evolutionary drivers underlying viral host jumps that may contribute to mitigating viral threats across species boundaries.

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Genomic screening of 16 UK native bat species through conservationist networks uncovers coronaviruses with zoonotic potential

Cited by 4 publications

References 112 publications

Survey of white-footed mice in Connecticut, USA reveals low SARS-CoV-2 seroprevalence and infection with divergent betacoronaviruses

Survey of white-footed mice in Connecticut, USA reveals low SARS-CoV-2 seroprevalence and infection with divergent betacoronaviruses

Detection and characterization of novel luchacoviruses, genusAlphacoronavirus, shed in saliva and feces of meso-carnivores in the northeastern United States

Crossing host boundaries: the evolutionary drivers and correlates of viral host jumps

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