AI Article Synopsis
- Viral encephalitides pose a serious threat to neonates due to inflammation-induced damage to the central nervous system (CNS), prompting this study to investigate proinflammatory cytokines' roles in managing viral replication and harmful immune responses.
- Neonatal mice infected with the arenavirus Tacaribe (TCRV) exhibited a severe form of meningoencephalitis, but neutralizing TNF-alpha led to reduced inflammation and improved survival outcomes, despite not clearing the virus.
- Combining anti-TNF-alpha antibodies with innate immune activators resulted in complete viral clearance and 100% survival, marking a significant advancement in therapeutic strategies for deadly viral infections affecting the nervous system.
Article Abstract
Viral encephalitides are life-threatening diseases in neonates partly due to the irreversible damage inflammation causes to the CNS. This study explored the role of proinflammatory cytokines in the balance between controlling viral replication and eliciting pathologic immune responses in nonlytic viral encephalitis. We show that neonatal mice challenged with arenavirus Tacaribe (TCRV) develop a meningoencephalitis characterized by high IFN-gamma and TNF-alpha levels and mild T cell infiltration. Neutralization of the TNF-alpha using mAb was associated with lower chemokine expression, reduced T cell infiltration, and lower levels of IFN-gamma, and TNF-alpha in the CNS and led to 100% survival. Moreover, treatment with Abs to TNF-alpha improved mobility and increased survival even after the mice developed bilateral hind limb paralysis. Of note, animals treated with anti-TNF-alpha Abs alone did not clear the virus despite generating Abs to TCRV. Direct activation of the innate immune response using CpG oligodeoxynucleotides in combination with anti-TNF-alpha Abs resulted in 100% survival and complete viral clearance. To our knowledge, this is the first demonstration of the use of innate immune modulators plus Abs to TNF-alpha as therapeutics for a lethal neurotropic viral infection.
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| http://dx.doi.org/10.4049/jimmunol.180.12.8231 | DOI Listing |
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