Literature detail

Structure-Guided Identification of a Nonhuman Morbillivirus with Zoonotic Potential.

Nurshariza Abdullah^1,2 James T Kelly¹ Stephen C Graham³ Jamie Birch¹ Daniel Gonçalves-Carneiro^1,2 Tim Mitchell² Robin N Thompson^4,5,6 Katrina A Lythgoe^4,7 Nicola Logan⁸ Margaret J Hosie⁸ Vassiliy N Bavro⁹ Brian J Willett⁸ Michael P Heaton¹⁰ Dalan Bailey^11,2

Affiliations 11 institutions

The Pirbright Institute, Surrey, United Kingdom.
The University of Birmingham, Birmingham, United Kingdom.
Department of Pathology, University of Cambridge, Cambridge, United Kingdom.
Department of Zoology, University of Oxford, Oxford, United Kingdom.
Mathematical Institute, University of Oxford, Oxford, United Kingdom.
Christ Church, University of Oxford, Oxford, United Kingdom.
Big Data Institute, University of Oxford, Oxford, United Kingdom.
MRC University of Glasgow Centre for Virus Research, Glasgow, United Kingdom.
School of Biological Sciences, University of Essex, Colchester, United Kingdom.
U.S. Meat Animal Research Center, Agricultural Research Service, U.S. Department of Agriculture, Clay Center, Nebraska, USA.
The Pirbright Institute, Surrey, United Kingdom [email protected].

PMID 30232185 2018 J Virol eng epublish

PubMed DOI Browse context

Article

Publication summary

Morbilliviruses infect a broad range of mammalian hosts, including ruminants, carnivores, and humans. The recent eradication of rinderpest virus (RPV) and the active campaigns for eradication of the human-specific measles virus (MeV) have raised significant concerns that the remaining morbilliviruses may emerge in so-called vacated ecological niches. Seeking to assess the zoonotic potential of nonhuman morbilliviruses within human populations, we found that peste des petits ruminants virus (PPRV)-the small-ruminant morbillivirus-is restricted at the point of entry into human cells due to deficient interactions with human SLAMF1-the immune cell receptor for morbilliviruses. Using a structure-guided approach, we characterized a single amino acid change, mapping to the receptor-binding domain in the PPRV hemagglutinin (H) protein, which overcomes this restriction. The same mutation allowed escape from some cross-protective, human patient, anti-MeV antibodies, raising concerns that PPRV is a pathogen with zoonotic potential. Analysis of natural variation within human and ovine SLAMF1 also identified polymorphisms that could correlate with disease resistance. Finally, the mechanistic nature of the PPRV restriction was also investigated, identifying charge incompatibility and steric hindrance between PPRV H and human SLAMF1 proteins. Importantly, this research was performed entirely using surrogate virus entry assays, negating the requirement for in situ derivation of a human-tropic PPRV and illustrating alternative strategies for identifying gain-of-function mutations in viral pathogens.IMPORTANCE A significant proportion of viral pandemics occur following zoonotic transmission events, where animal-associated viruses jump species into human populations. In order to provide forewarnings of the emergence of these viruses, it is necessary to develop a better understanding of what determines virus host range, often at the genetic and structural levels. In this study, we demonstrated that the small-ruminant morbillivirus, a close relative of measles, is unable to use human receptors to enter cells; however, a change of a single amino acid in the virus is sufficient to overcome this restriction. This information will be important for monitoring this virus's evolution in the field. Of note, this study was undertaken in vitro, without generation of a fully infectious virus with this phenotype.

host range measles morbillivirus paramyxovirus PPRV zoonoses Mutation Virus Replication Amino Acid Sequence Animals Antibodies, Viral Chlorocebus aethiops Glycoproteins Humans Models, Theoretical Mutagenesis, Site-Directed Peste-des-Petits-Ruminants Peste-des-petits-ruminants virus

Structured evidence records

Evidence records

2 total

Molecular Adaptation 1 records

Molecular Adaptation Extraction confidence 1.00

Key finding

A single amino acid mutation in the PPRV H protein receptor-binding domain enables use of human SLAMF1, overcoming entry restriction and enabling partial immune escape from anti-measles antibodies.

Virus

Host

Location

Supporting text

Using a structure-guided approach, we characterized a single amino acid change, mapping to the receptor-binding domain in the PPRV hemagglutinin (H) protein, which overcomes this restriction. The same mutation allowed escape from some cross-protective, human patient, anti-MeV antibodies, raising concerns that PPRV is a pathogen with zoonotic potential.

Genes or proteins: H
Receptors: SLAMF1
Mechanism types: receptor_binding; immune_escape

Receptor Usage 1 records

Receptor Usage Extraction confidence 1.00

Key finding

Peste des petits ruminants virus (PPRV) does not efficiently use human SLAMF1 for entry, but a single amino acid substitution in its hemagglutinin receptor-binding domain enables interaction and entry via this receptor.

Virus

Host

Location

Supporting text

We found that peste des petits ruminants virus (PPRV) is restricted at the point of entry into human cells due to deficient interactions with human SLAMF1, the immune cell receptor for morbilliviruses. Using a structure-guided approach, we characterized a single amino acid change, mapping to the receptor-binding domain in the PPRV hemagglutinin (H) protein, which overcomes this restriction.

Method: structure-guided approach; surrogate virus entry assays
Receptors: human SLAMF1

Citation context

References

60 references

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Evidence overview

Evidence 2

Types 2

Virus 1

Host 1

Evidence types

Molecular Adaptation 1 Receptor Usage 1

Linked entities

Viruses

Hosts

Locations

Publication metadata

Journal: Journal of virology
Volume / Issue / Pages: 92 / 23 / -
ISSN: 1098-5514
Journal country: United States
DOI: 10.1128/JVI.01248-18