Literature detail

Discovery and Genomic Characterization of a Novel Henipavirus, Angavokely Virus, from Fruit Bats in Madagascar.

Sharline Madera¹ Amy Kistler² Hafaliana C Ranaivoson^3,4,5 Vida Ahyong² Angelo Andrianiaina⁵ Santino Andry⁶ Vololoniaina Raharinosy⁴ Tsiry H Randriambolamanantsoa⁴ Ny Anjara Fifi Ravelomanantsoa⁵ Cristina M Tato² Joseph L DeRisi^2,7 Hector C Aguilar⁸ Vincent Lacoste⁴ Philippe Dussart⁴ Jean-Michel Heraud^4,9 Cara E Brook³

Affiliations 9 institutions

Division of Infectious Diseases, Department of Medicine, University of California, San Francisco, California, USA.
Chan Zuckerberg Biohub, San Francisco, California, USA.
Department of Ecology and Evolution, University of Chicagogrid.170205.1, Chicago, Illinois, USA.
Virology Unit, Institut Pasteur de Madagascar, Antananarivo, Madagascar.
Department of Zoology and Animal Biodiversity, University of Antananarivo, Antananarivo, Madagascar.
Department of Entomology, University of Antananarivo, Antananarivo, Madagascar.
Department of Medicine and Biochemistry & Biophysics, University of California, San Francisco, California, USA.
Department of Microbiology and Immunology, College of Veterinary Medicine, Cornell University, Ithaca, New York, USA.
Virology Department, Institut Pasteur de Dakargrid.418508.0, Dakar, Senegal.

PMID 36040175 2022 J Virol eng ppublish

PubMed DOI Browse context

Article

Publication summary

The genus Henipavirus (family Paramyxoviridae) currently comprises seven viruses, four of which have demonstrated prior evidence of zoonotic capacity. These include the biosafety level 4 agents Hendra (HeV) and Nipah (NiV) viruses, which circulate naturally in pteropodid fruit bats. Here, we describe and characterize Angavokely virus (AngV), a divergent henipavirus identified in urine samples from wild, Madagascar fruit bats. We report the nearly complete 16,740-nucleotide genome of AngV, which encodes the six major henipavirus structural proteins (nucleocapsid, phosphoprotein, matrix, fusion, glycoprotein, and L polymerase). Within the phosphoprotein (P) gene, we identify an alternative start codon encoding the AngV C protein and a putative mRNA editing site where the insertion of one or two guanine residues encodes, respectively, additional V and W proteins. In other paramyxovirus systems, C, V, and W are accessory proteins involved in antagonism of host immune responses during infection. Phylogenetic analysis suggests that AngV is ancestral to all four previously described bat henipaviruses-HeV, NiV, Cedar virus (CedV), and Ghanaian bat virus (GhV)-but evolved more recently than rodent- and shrew-derived henipaviruses, Mojiang (MojV), Gamak (GAKV), and Daeryong (DARV) viruses. Predictive structure-based alignments suggest that AngV is unlikely to bind ephrin receptors, which mediate cell entry for all other known bat henipaviruses. Identification of the AngV receptor is needed to clarify the virus's potential host range. The presence of V and W proteins in the AngV genome suggest that the virus could be pathogenic following zoonotic spillover. IMPORTANCE Henipaviruses include highly pathogenic emerging zoonotic viruses, derived from bat, rodent, and shrew reservoirs. Bat-borne Hendra (HeV) and Nipah (NiV) are the most well-known henipaviruses, for which no effective antivirals or vaccines for humans have been described. Here, we report the discovery and characterization of a novel henipavirus, Angavokely virus (AngV), isolated from wild fruit bats in Madagascar. Genomic characterization of AngV reveals all major features associated with pathogenicity in other henipaviruses, suggesting that AngV could be pathogenic following spillover to human hosts. Our work suggests that AngV is an ancestral bat henipavirus that likely uses viral entry pathways distinct from those previously described for HeV and NiV. In Madagascar, bats are consumed as a source of human food, presenting opportunities for cross-species transmission. Characterization of novel henipaviruses and documentation of their pathogenic and zoonotic potential are essential to predicting and preventing the emergence of future zoonoses that cause pandemics.

bat-borne virus Eidolon dupreanum emerging zoonosis henipavirus Madagascar novel virus Chiroptera Genome, Viral Henipavirus Henipavirus Infections Nipah Virus Animals Glycoproteins Humans Madagascar Phylogeny Urine Zoonoses

Structured evidence records

Evidence records

6 total

Molecular Adaptation 2 records

Molecular Adaptation Extraction confidence 0.85

Key finding

The Angavokely virus genome encodes C, V, and W accessory proteins via an edited phosphoprotein gene, which are associated with immune antagonism and may relate to pathogenic adaptation.

Virus

Host

Location

Supporting text

Within the phosphoprotein (P) gene, we identify an alternative start codon encoding the AngV C protein and a putative mRNA editing site where the insertion of one or two guanine residues encodes, respectively, additional V and W proteins. In other paramyxovirus systems, C, V, and W are accessory proteins involved in antagonism of host immune responses during infection.

Genes or proteins: phosphoprotein; C protein; V protein; W protein
Mechanism types: immune_escape; pathogenicity

Molecular Adaptation Extraction confidence 0.85

Key finding

Structural alignment analysis suggests the Angavokely virus glycoprotein does not bind ephrin receptors used by other henipaviruses, indicating possible differences in cell entry and host range.

Virus

Host

Location

Supporting text

Predictive structure-based alignments suggest that AngV is unlikely to bind ephrin receptors, which mediate cell entry for all other known bat henipaviruses.

Genes or proteins: glycoprotein
Receptors: ephrin receptors
Mechanism types: receptor_binding; cell_entry; host_range

Genomic Evolution 1 records

Genomic Evolution Extraction confidence 0.95

Key finding

Angavokely virus from fruit bats in Madagascar was found to have a nearly complete genome and is phylogenetically ancestral to other bat henipaviruses, indicating a distinct evolutionary lineage within the genus Henipavirus.

Virus

Host

Location

Supporting text

We report the nearly complete 16,740-nucleotide genome of AngV... Phylogenetic analysis suggests that AngV is ancestral to all four previously described bat henipaviruses-HeV, NiV, Cedar virus (CedV), and Ghanaian bat virus (GhV)-but evolved more recently than rodent- and shrew-derived henipaviruses.

Genes or proteins: nucleocapsid; phosphoprotein; matrix; fusion; glycoprotein; L polymerase; C; V; W
Analysis methods: genomic characterization; phylogenetic analysis

Receptor Usage 1 records

Receptor Usage Extraction confidence 0.80

Key finding

Angavokely virus appears unlikely to use ephrin receptors for cell entry, implying distinct receptor specificity from other bat henipaviruses.

Virus

Host

Location

Supporting text

Predictive structure-based alignments suggest that AngV is unlikely to bind ephrin receptors, which mediate cell entry for all other known bat henipaviruses.

Method: predictive structure-based alignment
Receptors: ephrin receptors

Reservoir Ecology 1 records

Reservoir Ecology Extraction confidence 0.75

Key finding

Angavokely virus was discovered in urine samples from wild fruit bats in Madagascar, indicating these bats serve as a natural reservoir.

Virus

Host

Location

Supporting text

We describe and characterize Angavokely virus (AngV), a divergent henipavirus identified in urine samples from wild, Madagascar fruit bats.

Method: field sampling; genomic characterization
Sample type: urine samples
Geographic raw: Madagascar
Country inferred: Madagascar

Zoonotic Surveillance 1 records

Zoonotic Surveillance Extraction confidence 0.95

Key finding

A divergent henipavirus, Angavokely virus, was discovered and genomically characterized from urine samples of wild fruit bats in Madagascar.

Virus

Host

Location

Supporting text

Here, we describe and characterize Angavokely virus (AngV), a divergent henipavirus identified in urine samples from wild, Madagascar fruit bats.

Method: genomic characterization
Sample type: urine
Geographic raw: Madagascar
Country inferred: Madagascar

Citation context

References

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Evidence overview

Evidence 6

Types 5

Virus 1

Host 1

Evidence types

Molecular Adaptation 2 Genomic Evolution 1 Receptor Usage 1 Reservoir Ecology 1 Zoonotic Surveillance 1

Linked entities

Viruses

Hosts

Locations

Publication metadata

Journal: Journal of virology
Volume / Issue / Pages: 96 / 18 / e0092122
ISSN: 1098-5514
Journal country: United States
DOI: 10.1128/jvi.00921-22