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CNS Recruitment of CD8+ T Lymphocytes Specific for a Peripheral Virus Infection Triggers Neuropathogenesis during Polymicrobial Challenge

Author: AE Denton
B Gran
C Consilvio
C Martin
CE Patterson
CE Patterson
Christine M. Matullo
CM Matullo
CR Mackay
D Kagi
D Masopust
D Papadimitriou
DH Gilden
DMP Lawrence
DMP Lawrence
EC Butcher
FM Marelli-Berg
G Lertmemongkolchai
GF Rall
GF Rall
Glenn F. Rall
H Okamura
J Nitcheu
JA Nathanson
JE Christensen
JE Christensen
JP Antel
K Moisse
KA Brogden
Kevin J. O'Regan
LO Bakaletz
M Buchmeier
M vonGeldern
Mark Curtis
MBA Oldstone
MJ Buchmeier
MP Walker
N Grigoriadis
N Weis
NT Joncker
NT Joncker
P Borrow
R Rochford
RE Berg
RE Berg
Robert E. Johnston
SA Sargsyan
SS Kang
TJ Chapman
WJ Streit
Y Shinkai
YH Huang
YJ Kim
Publication venue: Public Library of Science
Publication date: 01/12/2011
Field of study

Although viruses have been implicated in central nervous system (CNS) diseases of unknown etiology, including multiple sclerosis and amyotrophic lateral sclerosis, the reproducible identification of viral triggers in such diseases has been largely unsuccessful. Here, we explore the hypothesis that viruses need not replicate in the tissue in which they cause disease; specifically, that a peripheral infection might trigger CNS pathology. To test this idea, we utilized a transgenic mouse model in which we found that immune cells responding to a peripheral infection are recruited to the CNS, where they trigger neurological damage. In this model, mice are infected with both CNS-restricted measles virus (MV) and peripherally restricted lymphocytic choriomeningitis virus (LCMV). While infection with either virus alone resulted in no illness, infection with both viruses caused disease in all mice, with ∼50% dying following seizures. Co-infection resulted in a 12-fold increase in the number of CD8+ T cells in the brain as compared to MV infection alone. Tetramer analysis revealed that a substantial proportion (>35%) of these infiltrating CD8+ lymphocytes were LCMV-specific, despite no detectable LCMV in CNS tissues. Mechanistically, CNS disease was due to edema, induced in a CD8-dependent but perforin-independent manner, and brain herniation, similar to that observed in mice challenged intracerebrally with LCMV. These results indicate that T cell trafficking can be influenced by other ongoing immune challenges, and that CD8+ T cell recruitment to the brain can trigger CNS disease in the apparent absence of cognate antigen. By extrapolation, human CNS diseases of unknown etiology need not be associated with infection with any particular agent; rather, a condition that compromises and activates the blood-brain barrier and adjacent brain parenchyma can render the CNS susceptible to pathogen-independent immune attack

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