Document Type
Article
Publication Date
4-24-2014
Abstract
Central nervous system (CNS) metabolic profiles were examined from rabies virus (RABV)-infected mice that were either mock-treated or received post-exposure treatment (PET) with a single dose of the live recombinant RABV vaccine TriGAS. CNS tissue harvested from mock-treated mice at middle and late stage infection revealed numerous changes in energy metabolites, neurotransmitters and stress hormones that correlated with replication levels of viral RNA. Although the large majority of these metabolic changes were completely absent in the brains of TriGAS-treated mice most likely due to the strong reduction in virus spread, TriGAS treatment resulted in the up-regulation of the expression of carnitine and several acylcarnitines, suggesting that these compounds are neuroprotective. The most striking change seen in mock-treated RABV-infected mice was a dramatic increase in brain and serum corticosterone levels, with the later becoming elevated before clinical signs or loss of body weight occurred. We speculate that the rise in corticosterone is part of a strategy of RABV to block the induction of immune responses that would otherwise interfere with its spread. In support of this concept, we show that pharmacological intervention to inhibit corticosterone biosynthesis, in the absence of vaccine treatment, significantly reduces the pathogenicity of RABV. Our results suggest that widespread metabolic changes, including hypothalamic-pituitary-adrenal axis activation, contribute to the pathogenesis of RABV and that preventing these alterations early in infection with PET or pharmacological blockade helps protect brain homeostasis, thereby reducing disease mortality.
Recommended Citation
Schutsky, Keith; Portocarrero, Carla; Hooper, D Craig; Dietzschold, Bernhard; and Faber, Milosz, "Limited Brain Metabolism Changes Differentiate between the Progression and Clearance of Rabies Virus." (2014). Department of Microbiology and Immunology Faculty Papers. Paper 60.
https://jdc.jefferson.edu/mifp/60
Creative Commons License
This work is licensed under a Creative Commons Attribution 4.0 License.
PubMed ID
24763072
Comments
This article is the final published version in PLoS ONE Volume 9, Issue 9, April 2014, Article number e87180.
The published version is available at DOI: 10.1371/journal.pone.0087180. Copyright © Public Library of Science