The central nervous system inflammatory response to neurotropic virus infection is peroxynitrite dependent

D C Hooper; R B Kean; G S Scott; S V Spitsin; T Mikheeva; K Morimoto; M Bette; A M Röhrenbeck; B Dietzschold; E Weihe

doi:10.4049/jimmunol.167.6.3470

The central nervous system inflammatory response to neurotropic virus infection is peroxynitrite dependent

J Immunol. 2001 Sep 15;167(6):3470-7. doi: 10.4049/jimmunol.167.6.3470.

Authors

D C Hooper¹, R B Kean, G S Scott, S V Spitsin, T Mikheeva, K Morimoto, M Bette, A M Röhrenbeck, B Dietzschold, E Weihe

Affiliation

¹ Department of Microbiology and Immunology, Thomas Jefferson University, Philadelphia, PA 19107, USA. [email protected]

PMID: 11544340
DOI: 10.4049/jimmunol.167.6.3470

Abstract

We have recently demonstrated that increased blood-CNS barrier permeability and CNS inflammation in a conventional mouse model of experimental allergic encephalomyelitis are dependent upon the production of peroxynitrite (ONOO(-)), a product of the free radicals NO* and superoxide (O2*(-)). To determine whether this is a reflection of the physiological contribution of ONOO(-) to an immune response against a neurotropic pathogen, we have assessed the effects on adult rats acutely infected with Borna disease virus (BDV) of administration of uric acid (UA), an inhibitor of select chemical reactions associated with ONOO(-). The pathogenesis of acute Borna disease in immunocompetent adult rats results from the immune response to the neurotropic BDV, rather than the direct effects of BDV infection of neurons. An important stage in the BDV-specific neuroimmune response is the invasion of inflammatory cells into the CNS. UA treatment inhibited the onset of clinical disease, and prevented the elevated blood-brain barrier permeability as well as CNS inflammation seen in control-treated BDV-infected rats. The replication and spread of BDV in the CNS were unchanged by the administration of UA, and only minimal effects on the immune response to BDV Ags were observed. These results indicate that the CNS inflammatory response to neurotropic virus infection is likely to be dependent upon the activity of ONOO(-) or its products on the blood-brain barrier.

Publication types

Research Support, Non-U.S. Gov't
Research Support, U.S. Gov't, Non-P.H.S.

MeSH terms

Acute Disease
Animals
Antigens, Viral / immunology
Blood-Brain Barrier / drug effects*
Borna Disease / immunology*
Borna Disease / pathology
Borna Disease / virology
Borna disease virus / immunology*
Borna disease virus / physiology
Brain / immunology*
Brain / metabolism
Brain / pathology
Brain / virology
Brain Chemistry / drug effects
Chemotaxis, Leukocyte / drug effects
Chemotaxis, Leukocyte / physiology*
Encephalitis, Viral / immunology*
Encephalitis, Viral / pathology
Encephalitis, Viral / virology
Female
Free Radical Scavengers / pharmacology
Free Radical Scavengers / therapeutic use*
Free Radicals
Gene Expression Profiling
Immunocompetence
Inflammation
Lymphocyte Count
Nerve Tissue Proteins / analysis
Neurons / enzymology
Neuroprotective Agents / pharmacology
Neuroprotective Agents / therapeutic use*
Nitric Oxide Synthase / analysis
Nitric Oxide Synthase Type II
Oxidation-Reduction
Peroxynitrous Acid / physiology*
Polymerase Chain Reaction
Rats
Rats, Inbred Lew
T-Lymphocyte Subsets / drug effects
Tyrosine / analogs & derivatives*
Tyrosine / analysis
Uric Acid / pharmacology
Uric Acid / therapeutic use*
Virus Replication / drug effects

Substances

Antigens, Viral
Free Radical Scavengers
Free Radicals
Nerve Tissue Proteins
Neuroprotective Agents
Peroxynitrous Acid
Uric Acid
3-nitrotyrosine
Tyrosine
Nitric Oxide Synthase
Nitric Oxide Synthase Type II
Nos2 protein, rat