Literature detail

Role of the spike glycoprotein of human Middle East respiratory syndrome coronavirus (MERS-CoV) in virus entry and syncytia formation.

Zhaohui Qian^1,2 Samuel R Dominguez Kathryn V Holmes

Affiliations 2 institutions

Department of Microbiology, University of Colorado School of Medicine, Aurora, Colorado, United States of America
Institute of Pathogen Biology, Chinese Academy of Medical Sciences and Peking Union Medical College, Beijing, China.

PMID 24098509 2013 PLoS One eng epublish

Article

Publication summary

Little is known about the biology of the emerging human group c betacoronavirus, Middle East Respiratory Syndrome coronavirus (MERS-CoV). Because coronavirus spike glycoproteins (S) mediate virus entry, affect viral host range, and elicit neutralizing antibodies, analyzing the functions of MERS-CoV S protein is a high research priority. MERS-CoV S on lentivirus pseudovirions mediated entry into a variety of cell types including embryo cells from New World Eptesicus fuscus bats. Surprisingly, a polyclonal antibody to the S protein of MHV, a group a murine betacoronavirus, cross-reacted in immunoblots with the S2 domain of group c MERS-CoV spike protein. MERS pseudovirions released from 293T cells contained only uncleaved S, and pseudovirus entry was blocked by lysosomotropic reagents NH4Cl and bafilomycin and inhibitors of cathepsin L. However, when MERS pseudovirions with uncleaved S protein were adsorbed at 4°C to Vero E6 cells, brief trypsin treatment at neutral pH triggered virus entry at the plasma membrane and syncytia formation. When 293T cells producing MERS pseudotypes co-expressed serine proteases TMPRSS-2 or -4, large syncytia formed at neutral pH, and the pseudovirions produced were non-infectious and deficient in S protein. These experiments show that if S protein on MERS pseudovirions is uncleaved, then viruses enter by endocytosis in a cathepsin L-dependent manner, but if MERS-CoV S is cleaved, either during virus maturation by serine proteases or on pseudovirions by trypsin in extracellular fluids, then viruses enter at the plasma membrane at neutral pH and cause massive syncytia formation even in cells that express little or no MERS-CoV receptor. Thus, whether MERS-CoV enters cells within endosomes or at the plasma membrane depends upon the host cell type and tissue, and is determined by the location of host proteases that cleave the viral spike glycoprotein and activate membrane fusion.

Virus Internalization Animals Cell Line Cell Membrane Chlorocebus aethiops Coronavirus Endosomes Gene Deletion Gene Expression Gene Order Giant Cells HEK293 Cells Humans Hydrogen-Ion Concentration Lentivirus Mice Receptors, Virus Spike Glycoprotein, Coronavirus

Structured evidence records

Evidence records

3 total

Host Range Experiment 1 records

Host Range Experiment Extraction confidence 0.95

Key finding

MERS-CoV spike glycoprotein enabled pseudovirus entry into cells from multiple hosts, including bat embryo cells, showing cross-species entry capability.

Virus

Host

Location

Supporting text

MERS-CoV S on lentivirus pseudovirions mediated entry into a variety of cell types including embryo cells from New World Eptesicus fuscus bats.

Method: pseudovirus entry assay
Experimental system: pseudovirus assay

Molecular Adaptation 1 records

Molecular Adaptation Extraction confidence 0.85

Key finding

Cleavage of the MERS-CoV spike glycoprotein by host serine proteases or trypsin enables plasma membrane entry and syncytia formation, indicating protease-dependent molecular adaptation of viral entry mechanisms.

Virus

Host

Location

Supporting text

If S protein on MERS pseudovirions is uncleaved, then viruses enter by endocytosis in a cathepsin L-dependent manner, but if MERS-CoV S is cleaved, either during virus maturation by serine proteases or by trypsin, then viruses enter at the plasma membrane and cause massive syncytia formation even in cells that express little or no MERS-CoV receptor.

Genes or proteins: spike glycoprotein (S)
Host factors: cathepsin L; TMPRSS2; TMPRSS4; trypsin
Mechanism types: receptor_binding; cell_entry; tissue_tropism

Receptor Usage 1 records

Receptor Usage Extraction confidence 0.95

Key finding

MERS-CoV spike mediates cell entry by endocytosis dependent on cathepsin L when uncleaved, and by plasma membrane fusion triggered by TMPRSS2 or trypsin when cleaved.

Virus

Host

Location

Supporting text

MERS pseudovirions released from 293T cells contained only uncleaved S, and pseudovirus entry was blocked by lysosomotropic reagents NH4Cl and bafilomycin and inhibitors of cathepsin L. When 293T cells producing MERS pseudotypes co-expressed serine proteases TMPRSS-2 or -4, large syncytia formed at neutral pH, and the pseudovirions produced were non-infectious and deficient in S protein. These experiments show that uncleaved S facilitates endocytosis in a cathepsin L-dependent manner, while cleaved S enables plasma membrane entry via serine proteases.

Method: pseudovirus assay; protease inhibition; cell-entry assay
Receptors: MERS-CoV receptor
Host factors: cathepsin L; TMPRSS2; trypsin; serine proteases

Citation context

References

72 references

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Evidence overview

Evidence 3

Types 3

Virus 1

Host 3

Evidence types

Host Range Experiment 1 Molecular Adaptation 1 Receptor Usage 1

Linked entities

Viruses

Hosts

Locations

Publication metadata

Journal: PloS one
Volume / Issue / Pages: 8 / 10 / e76469
ISSN: 1932-6203
Journal country: United States
DOI: 10.1371/journal.pone.0076469