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Publication : Pseudovirus rVSVĪ”G-ZEBOV-GP Infects Neurons in Retina and CNS, Causing Apoptosis and Neurodegeneration in Neonatal Mice.

First Author  McWilliams IL Year  2019
Journal  Cell Rep Volume  26
Issue  7 Pages  1718-1726.e4
PubMed ID  30759384 Mgi Jnum  J:286909
Mgi Id  MGI:6390108 Doi  10.1016/j.celrep.2019.01.069
Citation  McWilliams IL, et al. (2019) Pseudovirus rVSVDeltaG-ZEBOV-GP Infects Neurons in Retina and CNS, Causing Apoptosis and Neurodegeneration in Neonatal Mice. Cell Rep 26(7):1718-1726.e4
abstractText  Zaire Ebola virus (ZEBOV) survivors experience visual and CNS sequelae that suggests the ZEBOV glycoprotein can mediate neurotropism. Replication-competent rVSVDeltaG-ZEBOV-GP vaccine candidate is generally well tolerated; however, its potential neurotropism requires careful study. Here, we show that a single inoculation of rVSVDeltaG-ZEBOV-GP virus in neonatal C57BL/6 mice results in transient viremia, neurological symptoms, high viral titers in eyes and brains, and death. rVSVDeltaG-ZEBOV-GP infects the inner layers of the retina, causing severe retinitis. In the cerebellum, rVSVDeltaG-ZEBOV-GP infects neurons in the granular and Purkinje layers, resulting in progressive foci of apoptosis and neurodegeneration. The susceptibility to infection is not due to impaired type I IFN responses, although MDA5(-/-), IFNbeta(-/-), and IFNAR1(-/-) mice have accelerated mortality. However, boosting interferon levels by co-administering poly(I:C) reduces viral titers in CNS and improves survival. Although these data should not be directly extrapolated to humans, they challenge the hypothesis that VSV-based vaccines are non-neurotropic.
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