Literature detail

Molecular recognition of human ephrinB2 cell surface receptor by an emergent African henipavirus.

Benhur Lee^1,2 Olivier Pernet³ Asim A Ahmed^4,5 Antra Zeltina⁶ Shannon M Beaty¹ Thomas A Bowden⁷

Affiliations 7 institutions

Department of Microbiology, Icahn School of Medicine at Mount Sinai, New York, NY 10029
[email protected] [email protected].
Department of Microbiology, Immunology, and Molecular Genetics, David Geffen School of Medicine at UCLA, Los Angeles, CA 90095
Division of Infectious Disease, Boston Children's Hospital, Boston, MA 02115
and.
Division of Structural Biology, Wellcome Trust Centre for Human Genetics, University of Oxford, Oxford OX3 7BN, United Kingdom.
Division of Structural Biology, Wellcome Trust Centre for Human Genetics, University of Oxford, Oxford OX3 7BN, United Kingdom [email protected] [email protected].

PMID 25825759 2015 Proc Natl Acad Sci U S A eng ppublish

Article

Publication summary

The discovery of African henipaviruses (HNVs) related to pathogenic Hendra virus (HeV) and Nipah virus (NiV) from Southeast Asia and Australia presents an open-ended health risk. Cell receptor use by emerging African HNVs at the stage of host-cell entry is a key parameter when considering the potential for spillover and infection of human populations. The attachment glycoprotein from a Ghanaian bat isolate (GhV-G) exhibits <30% sequence identity with Asiatic NiV-G/HeV-G. Here, through functional and structural analysis of GhV-G, we show how this African HNV targets the same human cell-surface receptor (ephrinB2) as the Asiatic HNVs. We first characterized this virus-receptor interaction crystallographically. Compared with extant HNV-G-ephrinB2 structures, there was significant structural variation in the six-bladed β-propeller scaffold of the GhV-G receptor-binding domain, but not the Greek key fold of the bound ephrinB2. Analysis revealed a surprisingly conserved mode of ephrinB2 interaction that reflects an ongoing evolutionary constraint among geographically distal and phylogenetically divergent HNVs to maintain the functionality of ephrinB2 recognition during virus-host entry. Interestingly, unlike NiV-G/HeV-G, we could not detect binding of GhV-G to ephrinB3. Comparative structure-function analysis further revealed several distinguishing features of HNV-G function: a secondary ephrinB2 interaction site that contributes to more efficient ephrinB2-mediated entry in NiV-G relative to GhV-G and cognate residues at the very C terminus of GhV-G (absent in Asiatic HNV-Gs) that are vital for efficient receptor-induced fusion, but not receptor binding per se. These data provide molecular-level details for evaluating the likelihood of African HNVs to spill over into human populations.

emerging virus glycoprotein henipavirus structure viral attachment Ephrin-B2 Henipavirus Viral Proteins Virus Internalization Ephrin-B3 HEK293 Cells Henipavirus Infections Humans Protein Structure, Quaternary Protein Structure, Secondary Protein Structure, Tertiary Structure-Activity Relationship

Structured evidence records

Evidence records

4 total

Receptor Usage 2 records

Receptor Usage Extraction confidence 1.00

Key finding

The Ghanaian bat isolate of African henipavirus (GhV-G) binds human ephrinB2 as its cell entry receptor, similar to Nipah and Hendra viruses.

Virus

Host

Location

Supporting text

Through functional and structural analysis of GhV-G, we show how this African HNV targets the same human cell-surface receptor (ephrinB2) as the Asiatic HNVs.

Method: functional analysis; structural analysis; crystallography
Receptors: ephrinB2

Receptor Usage Extraction confidence 1.00

Key finding

The African henipavirus GhV-G does not bind human ephrinB3, unlike other henipaviruses.

Virus

Host

Location

Supporting text

Unlike NiV-G/HeV-G, we could not detect binding of GhV-G to ephrinB3.

Method: binding assay
Receptors: ephrinB3

Genomic Evolution 1 records

Genomic Evolution Extraction confidence 0.80

Key finding

Comparative sequence and structural analysis showed that the Ghanaian bat henipavirus glycoprotein GhV-G is highly divergent from NiV-G and HeV-G but retains conserved ephrinB2 receptor recognition, indicating evolutionary conservation of receptor use among henipaviruses.

Virus

Host

Location

Supporting text

The attachment glycoprotein from a Ghanaian bat isolate (GhV-G) exhibits <30% sequence identity with Asiatic NiV-G/HeV-G. Comparative structure-function analysis revealed conserved ephrinB2 interaction reflecting an ongoing evolutionary constraint among geographically distal and phylogenetically divergent HNVs.

Genes or proteins: attachment glycoprotein (G)
Analysis methods: comparative sequence analysis; structural analysis

Molecular Adaptation 1 records

Molecular Adaptation Extraction confidence 0.95

Key finding

The attachment glycoprotein GhV-G of an African henipavirus exhibits structural adaptations in its receptor-binding domain that allow recognition of the human ephrinB2 receptor, maintaining functional entry while differing from NiV-G/HeV-G in binding and fusion efficiency.

Virus

Host

Location

Supporting text

Through functional and structural analysis of GhV-G, we show how this African HNV targets the same human cell-surface receptor (ephrinB2) as the Asiatic HNVs. Compared with extant HNV-G-ephrinB2 structures, there was significant structural variation in the six-bladed β-propeller scaffold of the GhV-G receptor-binding domain. A secondary ephrinB2 interaction site contributes to more efficient ephrinB2-mediated entry in NiV-G relative to GhV-G, and cognate residues at the very C terminus of GhV-G are vital for efficient receptor-induced fusion.

Genes or proteins: GhV-G; NiV-G; HeV-G
Receptors: ephrinB2; ephrinB3
Mechanism types: receptor_binding; cell_entry; pathogenicity

Citation context

References

72 references

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Evidence overview

Evidence 4

Types 3

Virus 1

Host 1

Evidence types

Receptor Usage 2 Genomic Evolution 1 Molecular Adaptation 1

Linked entities

Viruses

Hosts

Locations

Publication metadata

Journal: Proceedings of the National Academy of Sciences of the United States of America
Volume / Issue / Pages: 112 / 17 / E2156-65
ISSN: 1091-6490
Journal country: United States
DOI: 10.1073/pnas.1501690112