|
Immunization
With Neurofilament Light Protein Induces Spastic Paresis and Axonal
Degeneration in Biozzi ABH Mice.
Huizinga
R, Heijmans
N, Schubert
P, Gschmeissner
S, 't
Hart BA, Herrmann
H, Amor
S.
From
the Department of Immunobiology (RH, NH, PS, BAH, SA), Biomedical
Primate Research Centre, Rijswijk, The Netherlands; the EM unit (SG),
Cancer Research UK, London, UK; and the Division of Molecular Genetics (HH),
German Cancer Research Centre, Heidelberg, Germany.
Axonal
damage is the major cause of irreversible neurologic disability in
patients with multiple sclerosis. Although axonal damage correlates with
antibodies against neurofilament light (NF-L) protein, a major component
of the axonal cytoskeleton, the possible pathogenic role of autoimmunity
to axonal antigens such as NF-L has so far been ignored. Here we show
that Biozzi ABH mice immunized with NF-L protein develop neurologic
disease characterized by spastic paresis and paralysis concomitant with
axonal degeneration and inflammation primarily in the dorsal column of
the spinal cord. The inflammatory central nervous system lesions were
dominated by F4/80 macrophages/microglia and relatively low numbers of
CD4 and CD8 T-cells. In splenocyte cultures, proliferation to NF-L was
observed in CD4 T-cells accompanied by the production of the
proinflammatory cytokine interferon-gamma. Elevated levels of
circulating antibodies recognizing recombinant mouse NF-L were present
in the serum, and immunoglobulin deposits were observed within axons in
spinal cord lesions of mice exhibiting clinical disease. These data
provide evidence that autoimmunity to NF-L protein induces axonal
degeneration and clinical neurologic disease in mice, indicating that
autoimmunity to axonal antigens, as described in multiple sclerosis, may
be pathogenic rather than acting merely as a surrogate marker for axonal
degeneration.
PMID:
17413320 [PubMed - as supplied by publisher]
http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=pubmed&cmd=Retrieve&dopt=AbstractPlus&list_uids=17413320&itool=pubmed_DocSum |
