Neuroglia infection by rabies virus after anterograde virus spread in peripheral neurons.
Madlin PotratzLuca M ZaeckCarlotta WeigelAntonia KleinConrad M FreulingThomas MüllerStefan FinkePublished in: Acta neuropathologica communications (2020)
The highly neurotropic rabies virus (RABV) enters peripheral neurons at axon termini and requires long distance axonal transport and trans-synaptic spread between neurons for the infection of the central nervous system (CNS). Recent 3D imaging of field RABV-infected brains revealed a remarkably high proportion of infected astroglia, indicating that highly virulent field viruses are able to suppress astrocyte-mediated innate immune responses and virus elimination pathways. While fundamental for CNS invasion, in vivo field RABV spread and tropism in peripheral tissues is understudied. Here, we used three-dimensional light sheet and confocal laser scanning microscopy to investigate the in vivo distribution patterns of a field RABV clone in cleared high-volume tissue samples after infection via a natural (intramuscular; hind leg) and an artificial (intracranial) inoculation route. Immunostaining of virus and host markers provided a comprehensive overview of RABV infection in the CNS and peripheral nerves after centripetal and centrifugal virus spread. Importantly, we identified non-neuronal, axon-ensheathing neuroglia (Schwann cells, SCs) in peripheral nerves of the hind leg and facial regions as a target cell population of field RABV. This suggests that virus release from axons and infected SCs is part of the RABV in vivo cycle and may affect RABV-related demyelination of peripheral neurons and local innate immune responses. Detection of RABV in axon-surrounding myelinating SCs after i.c. infection further provided evidence for anterograde spread of RABV, highlighting that RABV axonal transport and spread of infectious virus in peripheral nerves is not exclusively retrograde. Our data support a new model in which, comparable to CNS neuroglia, SC infection in peripheral nerves suppresses glia-mediated innate immunity and delays antiviral host responses required for successful transport from the peripheral infection sites to the brain.
Keyphrases
- immune response
- chemotherapy induced
- spinal cord
- high resolution
- spinal cord injury
- blood brain barrier
- stem cells
- disease virus
- oxidative stress
- brain injury
- mesenchymal stem cells
- optical coherence tomography
- cell death
- cell cycle arrest
- cell therapy
- electronic health record
- high speed
- artificial intelligence
- raman spectroscopy
- peripheral nerve
- endoplasmic reticulum stress
- resting state
- electron microscopy
- fluorescence imaging
- subarachnoid hemorrhage
- cerebrospinal fluid