Enterovirus A71 crosses a human blood-brain barrier model through infected immune cells

Léa Gaume; Hélène Chabrolles; Maxime Bisseux; Igor Lopez-Coqueiro; Lucie Dehouck; Audrey Mirand; Cécile Henquell; Fabien Gosselet; Christine Archimbaud; Jean-Luc Bailly

doi:10.1128/spectrum.00690-24

Enterovirus A71 crosses a human blood-brain barrier model through infected immune cells

Microbiol Spectr. 2024 Jun 4;12(6):e0069024. doi: 10.1128/spectrum.00690-24. Epub 2024 May 16.

Authors

Léa Gaume¹, Hélène Chabrolles^{1

2}, Maxime Bisseux^{1

2}, Igor Lopez-Coqueiro¹, Lucie Dehouck³, Audrey Mirand^{1

2}, Cécile Henquell^{1

2}, Fabien Gosselet³, Christine Archimbaud^{1

2}, Jean-Luc Bailly¹

Affiliations

¹ Laboratoire Microorganismes: Génome et Environnement (LMGE), CNRS UMR 6023, Clermont Auvergne Université, Clermont-Ferrand, France.
² Laboratoire de Virologie, Centre National de Référence des Entérovirus et Parechovirus, CHU Clermont-Ferrand, Clermont-Ferrand, France.
³ Laboratoire de la Barrière Hémato-Encéphalique (LBHE), Université d'Artois, Lens, France.

PMID: 38752731
DOI: 10.1128/spectrum.00690-24

Abstract

Enterovirus A71 (EV-A71) is associated with neurological conditions such as acute meningitis and encephalitis. The virus is detected in the bloodstream, and high blood viral loads are associated with central nervous system (CNS) manifestations. We used an in vitro blood-brain barrier (BBB) model made up of human brain-like endothelial cells (hBLECs) and brain pericytes grown in transwell systems to investigate whether three genetically distinct EV-A71 strains (subgenogroups C1, C1-like, and C4) can cross the human BBB. EV-A71 poorly replicated in hBLECs, which released moderate amounts of infectious viruses from their luminal side and trace amounts of infectious viruses from their basolateral side. The barrier properties of hBLECs were not impaired by EV-A71 infection. We investigated the passage through hBLECs of EV-A71-infected white blood cells. EV-A71 strains efficiently replicated in immune cells, including monocytes, neutrophils, and NK/T cells. Attachment to hBLECs of immune cells infected with the C1-like virus was higher than attachment of cells infected with C1-06. EV-A71 infection did not impair the transmigration of immune cells through hBLECs. Overall, EV-A71 targets different white blood cell populations that have the potential to be used as a Trojan horse to cross hBLECs more efficiently than cell-free EV-A71 particles.IMPORTANCEEnterovirus A71 (EV-A71) was first reported in the USA, and numerous outbreaks have since occurred in Asia and Europe. EV-A71 re-emerged as a new multirecombinant strain in 2015 in Europe and is now widespread. The virus causes hand-foot-and-mouth disease in young children and is involved in nervous system infections. How the virus spreads to the nervous system is unclear. We investigated whether white blood cells could be infected by EV-A71 and transmit it across human endothelial cells mimicking the blood-brain barrier protecting the brain from adverse effects. We found that endothelial cells provide a strong roadblock to prevent the passage of free virus particles but allow the migration of infected immune cells, including monocytes, neutrophils, and NK/T cells. Our data are consistent with the potential role of immune cells in the pathogenesis of EV-A71 infections by spreading the virus in the blood and across the human blood-brain barrier.

Keywords: BBB crossing; EV-A71 neurotropism; blood–brain barrier model; neuroinvasion; white blood cells.

MeSH terms

Blood-Brain Barrier* / virology
Brain / virology
Endothelial Cells* / virology
Enterovirus A, Human* / genetics
Enterovirus A, Human* / physiology
Enterovirus Infections* / immunology
Enterovirus Infections* / virology
Humans
Killer Cells, Natural / immunology
Leukocytes / immunology
Leukocytes / virology
Monocytes / immunology
Monocytes / virology
Neutrophils / immunology
Neutrophils / virology
Pericytes / virology
Virus Replication

Grants and funding

OrganoVIR Grant 812673/EC | Horizon 2020 Framework Programme (H2020)